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OX F O R D A M E R I C A N PA I N L I B R A RY
Adjuvant Analgesics
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O A P L
OX F O R D A M E R I C A N PA I N L I B R A RY
Adjuvant Analgesics
Editedby
David Lussier,MD
Assistant Professor of Medicine
Institut universitaire de griatrie de Montral
University of Montral
Division of Geriatric Medicine and Alan-Edwards
Centre for Research in Pain
McGill University
Montral, Quebec,Canada
1
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From the use of opium poppy extracts and cannabis sativa millennia ago
to the development of novel analgesics, our knowledge of the pharmacology of pain has evolved considerably. Most of this improved knowledge
has occurred in the past few years. Indeed, improved understanding of the
mechanisms of pain at cellular, molecular, and synaptic levels has allowed
the development of analgesics acting on new targets, providing new hope
for better pain management and improved quality of life in millions of
patients worldwide.
There are many chapters and textbooks devoted to opioids but few on
other analgesics, the so-called adjuvant analgesics. These drugs include
analgesic antidepressants and anticonvulsants that are recommended as
first-line therapy for neuropathic pain (gabapentinoids, tricyclic antidepressants, duloxetine), cannabinoids, topical analgesics, local anesthetics, antihyperalgesics. We therefore felt that a new book was needed to fill a gap
in the literaturea book that would offer a comprehensive review of the
pharmacology of adjuvant analgesics that would be useful for clinicians and
clinical researchers, either physicians or other health professionals. To facilitate use for clinical purposes, we also included chapters on clinical entities
such as neuropathic pain, cancer pain, postoperative pain, and fibromyalgia.
Each chapter provides a detailed review of the current state of knowledge on a specific topic and offers a framework for considering future
developments on thattopic.
In preparing this book, we faced two main challenges. The first was to
cover a very broad area but still provide detailed information on each topic
for the practicing physician without exceeding a reasonable number of
pages. The second challenge we encountered was to provide reviews that
would still be timely after the book was published, given the rapid evolution of knowledge in this field. We are confident that we have succeeded
in meeting both challenges, mainly because all chapters were authored by
leading experts on the topic covered. We are very fortunate that we were
able to include so many world-renowned experts on the pharmacology
of pain in this book. We therefore extend our gratitude to all those who
agreed to take up the challenge of providing this state-of-the-art review of
such rapidly evolving fields. Our gratitude also goes to Andrea Knobloch
and all the Oxford University Press staff, for their patience and help during
the publication process. Finally, we thank Dr.Russell K.Portenoy, Editor of
this Oxford Pain series, for his guidance throughout the process.
Preface
Contents
Contributors ix
Classification of Analgesics
3 Antidepressants
C. Peter N.Watson
4 Anticonvulsants
David Lussier
5 Cannabinoids
33
Local Anesthetics
47
Patrick Friederich
59
Jana Sawynok
9.
Neuropathic Pain
79
NadineAttal
9.2
Cancer-related Pain
95
9.3
07
Mary-Ann Fitzcharles
9.4
Pierre Beaulieu
Index 47
Contributors
Laurent Bollag,MD
Associate Professor of
Anesthesiology and Pain Medicine
University of Washington
Seattle, Washington
Julie Desroches,PhD
Department of Pharmacology
Faculty of Medicine
University of Montreal
Montral, Canada
Mary-Ann Fitzcharles, MB,
ChB,FRCPC
Associate Professor of Medicine
Division of Rheumatology
McGill University; Alan Edwards
Pain ManagementUnit
McGill University HealthCenter
Montral, Quebec, Canada
Patrick Friederich,MD
Professor and Chairman of
Anesthesiology
Department of Anaesthesiology,
Critical Care Medicine, Pain Therapy
Bogenhausen Hospital
Academic Hospital of Technische
Universitt Mnchen
Munich, Germany
ix
CONTRIBUTORS
Cyril Rivat,PhD
Associate Professor
University of Montpellier
Institute of Neurosciences of
Montpellier (INM)-INSERM U05
Saint Eloi Hospital
Montpellier,France
Jana Sawynok,PhD
Department of Pharmacology
Dalhousie University
Halifax, Nova Scotia,Canada
C. Peter N.Watson,
MD,FRCPC
Assistant Professor of Medicine
University of Toronto
Toronto, Ontario,Canada
Chapter
Overview of Pain
Management
Pain, especially chronic persistent pain, is a multidimensional experience
defined as An unpleasant sensory and emotional experience associated with
actual or potential tissue damage, or described in terms of such damage
[]. As such, it responds better to a multimodal, multidimensional, interdisciplinary approach. Pain management should not only focus on decreasing the
noxious stimuli but also address the multiple dimensions and aim to minimize
impact on mood, function, and quality of life. To achieve these goals, treatment should combine nonpharmacological (physical, psychological), pharmacological, interventional, and specific approaches to pain management[2].
Nonpharmacological approaches
to pain management
Nonpharmacological approaches are traditionally categorized as physical and
psychological approaches.
Physical approaches include passive therapies such as transcutaneous
electrical nerve stimulation, ultrasounds, massage, and shock-wave therapies. Although these therapies can usually provide some short-term relief,
response is usually better and more sustained when active therapies are used,
such as exercises (aimed at increasing strength, tone, or flexibility) and rehabilitation practices. When managing pain, the goal should always be to ensure
that the patient has an active role and is fully involved in the therapeuticplan.
To achieve this goal, psychological approaches are used as an essential component of the pain-management strategy. Psychological approaches include
cognitive-behavioral therapy, strategies based on emotional disclosure, and
mind-body interventions (eg, yoga, mindfulness) [3]. The most appropriate
strategy for a given patient can be determined based on the nature and characteristics of the patients pain, comorbidities, personality traits, and previous
response to other treatments.
Interventional approaches
Interventional approaches to pain management include various techniques
aimed at reducing pain depending on the location and type of pain such
Specific approaches
Rather than treating pain, it is preferable to treat the cause of the pain, whenever possible. For example, the following surgeries may be performed to
treat pain:joint replacement in a patient with osteoarthritis, laminectomy and
fusion for a patient with spinal stenosis, and gamma knife ablation for patients
with trigeminal neuralgia.
Pharmacological approaches
The World Health Organization (WHO) Analgesic Ladder, first published in
2006, recommends treating pain based on severity [4](Figure .). Mild pain
should be treated with nonopioid analgesics (acetaminophen or nonsteroidal anti-inflammatory drugs), moderate pain should be treated with weak
opioids, and severe pain should be treated with strong opioids. Adjuvants
can be combined with analgesics for the treatment of pain of any severity,
depending on the nature of pain (see Chapter 2). Although it was first proposed for the treatment of cancer-related pain, the WHO pain ladder was
soon extrapolated to chronic nonmalignantpain.
Several authors have proposed modifications to the WHO pain ladder
in recent years, due to developing scientific evidence. Eisenberg etal [5]
Freedom from
cancer pain
Opioid for moderate to severe pain
+/ Non opioid
+/ Adjuvant
Pain persisting
or increasing
2
proposed to eliminate weak opioids for the treatment of cancer pain, because
low doses of strong opioids have been shown to provide better and faster
pain relief, with greater patient satisfaction [6]. Invasive procedures should be
considered at any stage, as an alternative or an adjunct to pharmacotherapy.
Vargas-Schaffer [7]proposed to keep steps 3 unchanged and add a
fourth step for managing the crises of chronic pain, comprising nerve block,
epidurals, patient-controlled analgesia pump, neurolytic block therapy, and
spinal stimulators. The treatment should also be adapted to the nature and
acuteness of pain, using a step up approach for chronic pain, nonmalignant
pain, and cancer pain and a step down approach for acute pain, chronic pain
without control, and acute crises of chronicpain.
Although evidence is still limited, there is proof that pain is better controlled, with fewer adverse effects, when using a combination of diverse
classes of analgesics [8](see Chapter 4 for examples). It is clinical experience derived from clinical practice. Therefore, when clinicians select the most
appropriate analgesics for a given patient, they should combine various analgesics with different mechanisms of action for a better pain relief.
Acetaminophen is recommended as first-line therapy to treat mild to moderate pain, especially of musculoskeletal origin, because of the rarity of toxicity
and adverse effects when used at therapeutic doses. Recent evidence and
most guidelines recommend a maximal daily dose of 3200 mg when acetaminophen is used for more than 0days in patients with risk factors for toxicity and 2600 mg in patients with other risk factors (polypharmacy, advanced
age, alcohol abuse, liver impairment). When used to treat acute pain of less
than 0-day duration, the traditional 4000 mg maximal daily dose can be used.
When acetaminophen is administered on a chronic basis, frequent monitoring
of liver function tests should be done to avoid liver toxicity.
Nonsteroidal anti-inflammatory drugs and selective cyclooxygenase-2
inhibitors are indicated for the treatment of inflammatory diseases
(eg, rheumatoid arthritis) or for the treatment of acute pain. Nonsteroidal
anti-inflammatory drugs are associated with significant adverse effects, including acute kidney injury, hyperkalemia, gastric toxicity, fluid retention, congestive heart failure, and possibly increased cardiac mortality; therefore, they
should be used with caution, especially in older patients or those with several
comorbidities or polypharmacy, with frequent monitoring for the occurrence
of adverse effects.
Opioids
As indicated earlier, opioids should be used for the treatment of pain of
moderate or severe intensity. Treatment should be initiated with a low dose
and increased progressively based on analgesic response and tolerability.
Responses to various opioids can vary depending on the patient and type of
Nonopioid analgesics
pain. Opioid rotation can be done when pain does not respond to a specific
opioid. When prescribing an opioid, it is always important to first evaluate
the risk of medication abuse and diversion and then frequently reassess these
issues.
Conclusion
This chapter provides a very brief overview of pain management. To ensure
optimal pain management, a combination of various pain relief strategies
should be used, with a multimodal and interprofessional approach, combining nonpharmacological, pharmacological, interventional, and specific
approaches. Pharmacotherapy should also include various classes of analgesics with different mechanisms of action, for better pain relief and tolerability.
References
. Merskey H, Bogduk N, eds. Classification of Chronic Pain, Second Edition. Seattle,
WA:IASP Press;994.
2. American Society of Anesthesiologists Task Force on Chronic Pain Management,
American Society of Regional Anesthesia and Pain Medicine. Practice guidelines
for chronic pain management:an updated report by the American Society of
Anesthesiologists Task Force on Chronic Pain Management and the American
Society of Regional Anesthesia and Pain Medicine. Anesthesiology 200;
2:80833.
3. Keefe FJ, Porter L, Somer T, etal. Psychosocial interventions for managing
pain in older adults:outcomes and clinical implications. Br J Anaesth 203;
:8994.
4. World Health Organization. WHOs pain ladder. Available at:www.who.int/
cancer/palliative/painladder/en/. Accessed 9 September204.
5. Eisenberg E, Marinangeli F, Birkhahm J, et al. Time to modify the WHO analgesic
ladder? Pain Clin Update 2005; 3:4.
6. Marinangeli F, Ciccozzi A, Leonardis M, etal. Use of strong opioids in advanced
cancer pain:a randomized trial. J Pain Symptom Manage 2004; 27:40946.
7. Vargas-Schaffer G. Is the WHO analgesic ladder still valid? Twenty-four years of
experience. Can Fam Physician 200; 56:5457.
8. Chaparro LE, Wiffen PJ, Moore RA, Gilron I. Combination pharmacotherapy
for the treatment of neuropathic pain in adults. Cochrane Database Syst Rev
202; 7:CD008943.
Chapter2
Classification of Analgesics
David Lussier and Pierre Beaulieu
Classification of Analgesics
Chapter2
Classification of Analgesics
Chapter2
Classification of Analgesics
Chapter2
Nociceptive
Neurogenic
Mechanisms
Somatic
(tissue injury)
Mechanical,
thermal, or
chemical stimuli
Visceral
(irritable bowel,
cystitis)
Inflammatory
(musculoskeletal)
Visceral
distension
Causalgia
(neuralgia,
radiculopathy, CNS
lesions)
Functional
(fibromyalgia,
thalamic syndromes,
irritable bowel)
Example of
Pharmacologic
Treatments
Acetaminophen
Sodium channel
blockers
NSAIDs
Steroids
Opioids
NSAIDs
Antispasmodics
Associated
with localized
inflammation
Peripheral or
CNS lesions
NSAIDs
Steroids
Dysregulation
of excitatory
or inhibitory
mechanisms in
CNS
Antidepressants
Anticonvulsants
Opioids
Cannabinoids
Anticonvulsants
Opioids
Antidepressants
Drug
Capsaicin
TTXs Na+-VGSC
TTXr Na+ -VGSC
Sympathetically
maintained pain
Central sensitization
-receptor
Sodium channel
blockers
Carbamazepine
Lamotrigine
Mexiletine
Lidocaine
Phentolamine
Guanethidine block
NMDA antagonists
Ketamine
Dextromethorphan
COX-2 selective
inhibitors
-opioid agonists,
gabapentin, clonidine,
tricyclic antidepressants
NMDA receptor
COX-2
Reduced inhibition
Increased
transmission
Receptors
MOR, 2, GABA,
N-type
Ca2+ channels
(continued)
Classification of Analgesics
Target
TRPV
Chapter2
Mechanism
Peripheral
sensitization
Ectopic discharge
Classification of Analgesics
Chapter2
Table2.6Continued
SSRIs
2-adrenergic agonists
Modulators of Peripheral Transmission or Sensitization
Local anesthetics
Carbamazepine
Oxcarbazepine
Topiramate
Capsaicin
Mixed:Antinociceptive Analgesics and Modulators of Descending Inhibition
or Excitation
Tramadol
Tapentadol
Other
Calcitonin
Bisphosphonates
10
References
. World Health Organization. WHOs pain ladder. Available at:www.who.int/
cancer/palliative/painladder/en/. Accessed 29 August204.
2. World Health Organization. Treatment guidelines on pain related to
cancer, HIV and other progressive life-threatening illnesses in adults.
Adopted in WHO Steering Group on Pain Guidelines, October 4, 2008.
Available at: http://www.who.int/medicines/areas/quality_safety/
Scoping_WHOGuide_non-malignant_pain_adults.pdf. Accessed 8
November,204.
3. Lussier D, Portenoy RK. Adjuvant analgesics in pain management. In:Hanks
G, Cherny N, Christakis N, etal, eds. Oxford Textbook of Palliative Medicine,
4th edition. Oxford, England:Oxford University Press, 200; pp. 707734.
4. Lussier D, Beaulieu P. Toward a rational taxonomy of analgesics. In:Beaulieu P,
Lussier D, Porreca F, Dickenson AH, eds. Pharmacology of Pain. Seattle, WA:IASP
Press, 200; pp.2740.
5. Marchand S. The physiology of pain mechanisms:from the periphery to the
brain. Rheum Dis Clin North Am 2008; 34:285309.
6. Costigan M, Woolf CJ. Pain:molecular mechanisms. J Pain 2000; (Suppl ):3544.
Chapter3
Antidepressants
C. Peter N.Watson
I do believe, said Alice at last, that they live in the same house!
LEWIS CARROLL, Through the LookingGlass
The quotation refers to both the independent analgesic action and the dual
action on inhibitory monoaminergic neurotransmitters of some antidepressants. Antidepressants are one of the oldest pharmacological treatments for
chronic pain, and they have been subjected to many randomized controlled
trials (RCTs) for chronic noncancer pain (CNCP) []. More than a quarter
century of investigation has resulted in a large amount of literature on this
topic. This chapter is based on systematic reviews of quality RCTs in chronic
non-cancer pain [5]. Historically, these RCTs first examined tricyclic antidepressants (TCAs) such as amitriptyline based on published observational
data and because of their putative action on potentiating pain-inhibitory
mechanisms involving serotonin and noradrenaline. Because of limitations
in efficacy and concern about adverse effects, attention turned to the more
selective serotonin re-uptake inhibitors (SSRIs) such as fluoxetine and others
and the more noradrenergic (N) agents such as maprotiline, desipramine, and
nortriptyline. More recently, because of disappointing results regarding the
superiority of most of these more specific antidepressants (except the more
N TCA nortriptyline [6]), recent research has explored new drugs such as the
serotonin noradrenaline re-uptake inhibitors (SNRIs) venlafaxine, duloxetine,
and milnacipran, which, similar to amitriptyline, have an effect on both serotonin and noradrenaline with the hope of fewer adverse effects and better
analgesia.
This chapter reviews () pharmacological aspects (dose, duration, pharmacodynamics, adverse effects) of these drugs (Table 3.) and (2) the
evidence-based data concerning clinical meaningfulness regarding efficacy
and safety in CNCP (arthritis, fibromyalgia [FM], headache, low back pain,
miscellaneous chronic pain, and particularly neuropathic pain [NP]) (Table
3.2). The TCAs, SSRIs, and combined SNRIs are considered here. There is
evidence of an analgesic action of some of the antidepressants by RCTs and
the relief of different components of NP in particular; that is, steady pain,
jabbing, and evoked pain (allodynia). Other analgesics can now be regarded
11
11
Introduction
12
Chapter3
Antidepressants
Therapeutic
Range for
Pain
(mg/24 h)
Half-life (h)
Tricyclics
Amitriptyline
050*
Doxepin
050*
Trimipramine
5-HT
046
+++
+++
>30
>0
>30
>30
>0
>2
836
+++
++
>30
>0
>0
>30
>0
<2
050*
730
++
>30
>0
>0
>0
>0
<2
Imipramine
050*
434
+++
+++
>0
>30
>0
>30
>0
>0
Clomipramine
050*
737
+++
++++
>2
>0
>0
>30
>0
>0
Desipramine
050*
276
+++++
++
>2
>2
>2
>0
>2
>2
Nortriptyline
000*
388
++++
++
>2
>2
>2
>0
>0
<2
++
++++
>0
>0
<2
>0
>0
>30
+++++ >0
<0
<2
>0
>0
>0
Duloxetine
Cymbalta
6020
93
(metabolite)
0
++++
NNT
Benefit
NNT Minor
Harm
3
No dichotomous 8.7
data available
8.9
7
Amitriptyline
Imipramine
Desipramine
Nortriptyline
Clomipramine
2.4
2.
2.4
2.6
2.
Average TCAs
2.3
Venlafaxine
4.0
SSRIs
6.7
Antidepressants
Agent*
Chapter3
This column refers to the number of studies for which there was adequate information with
which to calculate an average NNT. Please note that these figures derive from studies using
different methodologies, different data analyses, with different numbers of patients. There are
few comparative trials, and the external validity may be poor because of selection that goes into
trials. Thus, the NNT data are a rough guideonly.
+
Mechanism ofaction
Randomized controlled trials have repeatedly and clearly demonstrated the
separation of the analgesic and antidepressant effects [6,7]. An early concept of the mechanism of antidepressant analgesia was that this analgesia
occurred via pain-inhibiting systems that descend from the brainstem on to
the dorsal horn of the spinal cord [8]. This model involves an endorphin
13
**Major harm consists of withdrawal from the study due to adverse effects.
Antidepressants
Chapter3
14
link from the periaqueductal gray area to the medullary raphe nucleus and
then an S connection from the raphe to the dorsal horn of the spinal cord.
However, another inhibitory system extends from the locus coeruleus in the
lateral pons to the dorsal horn, which involves noradrenalin. More recently,
descending facilitation by an S mechanism has been described [9]. This may
explain the lesser or lack of efficacy of selective S drugs such as the SSRIs.
Randomized controlled trials have demonstrated that the selective S drugs
are either not effective [20] or less effective than N agents and those with
a mixed effect on S and N (TCAs, SNRIs). The more effective antidepressants for chronic pain seem to be the TCAs desipramine, amitriptyline and its
metabolite nortriptyline. Antidepressants are relatively dirty drugs that act
on multiple receptors and have multiple effects (dopamine potentiation, the
anticholinergic effect, an antihistaminic effect, an anti-inflammatory effect due
to the inhibition of prostaglandin synthetase, an opioid-mediated effect, K+
channel activation, GABAB potentiation, substance P reduction, or a calcium
channel blocking action). Recent attractive ideas, in light of current thinking,
are that these drugs may be N-methyl-D -aspartate antagonists or sodium
channel blockers. In this chapter, we will focus on the monoamine descending
inhibition model and use this model to categorize and explain the efficacy of
the analgesic antidepressants. Aggressive pharmaceutical marketing of newer
SNRI antidepressants for both NP and FM has created an impression among
clinicians that those are the first-line pharmacotherapy for these indications;
however, the evidence base does not support this assertion[7].
Acute and cancerpain
Use of antidepressants for acute and cancer pain is discussed in Chapters 9.4
and 9.2, respectively, as well as in Reference [].
Neuropathicpain
The definition, assessment methods, and most common etiologies of NP are
provided in Chapter 9.1. Most antidepressant research has been carried out
in NP, and 80% of NP RCTs have been done in painful diabetic neuropathy
(PDN) and postherpetic neuralgia (PHN). Sixty-one RCTs of 20 antidepressants in NP were identified []. Seventeen were conducted in PDN, in
PHN, and 33 in other NP conditions, which included facial pain, NP with cancer, central poststroke pain, human immunodeficiency virus (HIV) neuropathy, spinal cord injury, cisplatin neuropathy, painful polyneuropathy, phantom
limb pain, and chronic lumbar root pain. Of the trials of oral drugs, 3 antidepressants in 36 RCTs showed a significant effect. With TCAs, six drugs tested
favorably, including amitriptyline, imipramine, nortriptyline, desipramine, and
nortriptyline. Of SNRIs, venlafaxine and duloxetine were superior to placebo.
Selective serotonin re-uptake inhibitors yielded favorable results over placebo
with paroxetine, citalopram, and escitalopram. The tetracyclic, N maprotiline
(3 RCTs), and the N/dopaminergic bupropion (one RCT) also have shown a
significant effect compared with placebo. These RCTs have repeatedly shown
an analgesic effect independent of an effect on depression and the relief of
the different pain qualities seen in NP, including steady pain, jabbing pain, and
skin pain (allodynia or pain on touch). Randomized controlled trials results in
Antidepressants
Chapter3
PDN and PHN are reasonably similar, but negative trials in such NP disorders
as lumbar root pain, HIV and cisplatin neuropathies, and spinal cord injury
may reflect the greater intractability of these NP problems.
A significant difficulty for the clinician lies in interpreting the results of these
many RCTs for translation to clinical practice in deciding which drug to use.
One problem is the lack of clinical meaningfulness data in most studies such
as the number of subjects with satisfactory relief [5]. Another issue is the
paucity of comparative data (most RCTs are a comparison with placebo) [8].
To address these deficiencies, NNT figures for 50% or more relief and NNH
figures for withdrawal for NP RCTs have been calculated for both antidepressants and other analgesic classes [3] (Table 3.2). In NP, these data indicate
that balanced N/S TCAs are superior to N TCAs and SNRIs, which in turn
are superior to SSRIs. In addition, TCA NNTs are about equal to the opioids
morphine and oxycodone and superior to gabapentinoids (gabapentin, pregabalin), the opioid-like drug tramadol, and cannabinoids. These data are helpful in placing the different drugs in a treatment algorithm for NP [9], which
places TCAs as a first choice along with gabapentinoids and SNRIs as a second
choice.
Headache
Four antidepressants were favorable in 6 RCTs in tension-type headache,
migraine, and medication-induced and chronic daily headache [,4]. Of the
commercially available drugs, those with a mixed effect on serotonin and noradrenaline (ie, amitriptyline, venlafaxine, and mirtazapine) were superior in
both migraine and tension headache, but amitriptyline was superior in only
one RCT in drug withdrawal headache. The SSRIs were found to be no more
15
Fibromyalgia
Antidepressants
Chapter3
effective than placebo in migraine and less effective than TCAs in chronic
tension-type headaches [,4]. Thus, the TCA amitriptyline, the tetracyclic
mirtazapine, and the SNRI venlafaxine all seem useful for headache prevention of both migraine and tension-type headaches. Most RCTs report a reduction in duration and frequency of headache and, less commonly, of severity.
Low backpain
Three antidepressants were favorable for low back pain (amitriptyline, nortriptyline, and doxepin) [,3].
Arthritis
Amitriptyline, imipramine, and trimipramine were found to be favorable for
different arthritis conditions (osteoarthritis, rheumatoid arthritis, ankylosing
spondylitis)[].
16
Adverseevents
Table 3. summarizes monoamine profiles and common side effects for some
commonly used antidepressants, and more details are available elsewhere
[,23]. If insomnia accompanies pain, a sedating TCA may be chosen (such
as amitriptyline) and given in a single nightime dose, which may also mitigate
unwanted daytime drowsiness. The presence of a seizure disorder precludes
the use of bupropion. Allergic reactions are generally uncommon. Withdrawal
reactions may occur and gradual withdrawal is prudent. Number-needed-toharm figures for TCAs do not indicate a worse side-effect profile in RCTs
than other drug choices for CNCP such as gabapentinoids (Table 3.2) [3].
Most SNRIs are unlikely to cause severe anticholinergic, adrenergic, and antihistaminic side effects, severe sedation, hypotension, and weight gain. They
may cause gastrointestinal upset (commonest), insomnia, dry mouth, drowsiness, sweating, anxiety, agitation, headache, sexual dysfunction, and tremor.
Acentral S syndrome and an increased risk of gastrointestinal bleeding have
been reported. Serotonin norepinephrine re-uptake inhibitors may aggravate
hypertension, exacerbate seizures, and trigger mania. More common are nausea, anorexia, weakness, drowsiness, nervousness, dizziness, and dry mouth.
Drug interactions are a consideration with all antidepressants, and the safety
of most antidepressants in pregnancy and lactation has not been established.
Drug Selection
There are numerous largely placebo-controlled RCTs in CNCP, indicating
that a variety of antidepressants are superior to placebo in many conditions.
These trials may leave the clinician in a state of confusion as to the appropriate choice of agent because there are few head-to-head comparative trials
Approach to therapy
In selecting an antidepressant such as a TCA for CNCP, it is important to
() individualize therapy, (2) obtain a complete assessment, and (3) focus
Antidepressants
Chapter3
17
Antidepressants
Chapter3
18
on issues that may preclude these drugs such as advanced age, heart disease
(recent myocardial infarction, conduction defects), urinary retention, glaucoma, other medications, and alcohol intake. In deciding on antidepressant
therapy, a history of failed antidepressant usage should not dissuade one from
a careful trial because many failures result from high initial dosing, noncompliance, or an inadequate trial (too low a dose or too brief a trial). It is important
to carefully explain the goals of treatment and adverse effects to patients.
They need to understand that complete relief is possible but unlikely and
that the aim of treatment is to take the pain from severe or moderate to mild
(occurs in 50%60% in RCTs). Patients also need to know that the starting
dose will be low and will be slowly increased (every week or so) until satisfactory relief occurs or an intolerable adverse effect is experienced. It is important to inform them that the effect of a dose increase may not be experienced
for one week or more and that, if stopped, side effects are probable (the most
common with TCAs being dry mouth, constipation, and drowsiness) and that,
if stopped, drug withdrawal should be gradual. A sedating TCA (amitriptyline)
may be useful with the total dose at bedtime if insomnia is a problem or to
avoid daytime drug-induced drowsiness. Weight gain may occur with some
agents, in which case diet and appropriate weight monitoring are important,
particularly in the already overweight population. Sexual dysfunction may be
more important in the younger age groups. Less common adverse effects
are allergic reactions such as rash, tachycardia (usually supraventricular), and
paradoxical insomnia. If possible, it is prudent to eliminate all other ineffective
analgesics and sedating drugs so that drug interactions (such as sedation and
constipation) are minimized. Antidepressants may interact with other nonanalgesics such as those that either prolong the QT interval (eg, methadone)
or interfere with hepatic metabolism (via cytochrome P450), possibly causing ventricular tachycardia (antiarrythmics, antiretrovirals, antifungals, calcium
channel blockers, macrolide and quinolone antibiotics, SSRIs, antipsychotics,
tamoxifen, and cisapride) (see Chapter 10).
Useful baseline tests are blood pressure measurement supine and standing, hematology, liver and kidney function, electrolytes, and an electrocardiogram. Agood general principle is to start low and go slow, keeping
in mind that with TCAs the analgesic effect occurs at lower doses than the
antidepressant effect (mean, 5075 mg). If treatment is started with a TCA
such as nortriptyline (less significant adverse events) or amitriptyline, it is
reasonable to begin with 0 mg for patients over 65 and 25 mg for those
under 65 and then slowly increase the dose every week or two by similar
amounts until an end point of satisfactory pain relief or a significant adverse
event. It may be helpful to try different antidepressants and move from TCAs
(nortriptyline, amitriptyline, desipramine, imipramine) to the SNRIs (venlafaxine and duloxetine) because individual differences in pain inhibitory mechanisms may mean that one drug is more efficacious for an individual patient.
In addition, close follow-up (every 2 weeks initially) is important to supervise
compliance, dose increments, and to deal with adverse effects. Preemptive
prescription of a stool softener and an artificial saliva mouth spray are useful
routine measures. There is no therapeutic range of blood levels for antidepressants, but they can be useful to check compliance and as a guide to dose
Antidepressants
Chapter3
This chapter provides information about the pharmacology of antidepressants, guidelines and data regarding efficacy and safety from recent systematic
reviews concerning antidepressants and pain and individual quality RCTs. Of
particular interest in these studies are the clinical meaningfulness of the results
and how the drugs compare with the standard therapy of the more specific
subclass of TCAs and other analgesics. An important concern is the limited
external validity or generalizability of trial data to the same disorders in ordinary practice. There are few head-to-head RCTs that compare different antidepressants with other analgesics. Indirect comparative measures such as
NNT and NNH values are a useful additional means of comparison. Despite
the increase in placebo-controlled RCTs of antidepressants in painful conditions, there has been no striking advance or magic bullet for monotherapy.
There continues to be a need for comparative effectiveness research of new
antidepressants by quality head-to-head RCTs comparing new drugs with old
drugs to guide the clinician. Because of deficiencies in this area and because of
evidence for poor generalizability, combinations of the useful antidepressants
with other analgesic drugs need to be considered for many patients.
References
. Watson CPN, Gilron I, Pollock BG, Lipman AG, Smith MT. Antidepressant
analgesics. In:McMahon JR, Koltzenburg M, Tracey I, and Turck DC (eds.)
Wall and Melzacks Textbook of Pain, 6th ed. Elsevier/Churchill Livingstone;
202:pp. 465490.
2. Saarto T, Wiffen PJ. Antidepressants in neuropathic pain (Review). The
Cochrane Collaboration. The Cochrane Library:John Wiley & Sons Ltd.
Available at: http://onlinelibrary.wiley.com/doi/0.002/465858.
CD005454.pub2/abstract. 2007. Accessed 9 November,204.
3. Urquhart DM, Hoving JL, Assendelft WJ, etal. Antidepressants for non-specific
low back pain (Review). The Cochrane Collaboration. The Cochrane
Library:John Wiley & Sons, Ltd. Available at:http://onlinelibrary.wiley.com/
doi/0.002/465858.CD00703.pub3/abstract.2008.
4. Moja L, Cusi C, Sterzi R, etal. Selective serotonin re-uptake inhibitors for
preventing migraine and tension headaches (Review). The Cochrane
Collaboration. The Cochrane Library: John Wiley & Sons Ltd. Available
19
Summary
Antidepressants
Chapter3
20
at: http://onlinelibrary.wiley.com/doi/0.002/465858.CD00299.
pub2/abstract. 2005. Accessed 9 November,204.
5. Lynch ME, Watson CP. The pharmacotherapy of chronic pain:a review. Pain
Res Manag 2006; :38.
6. Watson CP, Vernich L, Chipman M, Reed K. Nortriptyline versus amitriptyline
in postherpetic neuralgia:a randomized trial. Neurology 998; 5:667.
7. Watson CP, Gilron I, Sawynok J, Lynch ME. Nontricyclic antidepressants and
pain:are the serotonin norepinephrine reuptake inhibitors any better? Pain
20; 52:2206220.
8. Watson CP, Gilron I, Sawynok J. A qualitative, systematic review of head-tohead randomized, controlled trials of oral analgesics in neuropathic pain. J Pain
Res Manag 200; 5:4757.
9. Moulin DE, Clark AJ, Gilron I, etal. Pharmacological management of chronic
neuropathic pain-consensus statement and guidelines from the Canadian pain
Society. Pain Res Manag 2007; 2:32.
0. Dworkin RH, OConnor AB, Backonja M, et al. Pharmacologic management of neuropathic pain: evidence-based recommendations. Pain 2007;
32:23725.
. Attal N, Cruccu G, Baron R, etal. EFNS guidelines on the pharmacological
treatment of neuropathic pain:200 revision. Eur J Neur 200; 7:323.
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3. Finnerup NB, Sindrup SH, Jensen TS. The evidence for pharmacological treatment of neuropathic pain. Pain 200; 50:57358.
4. Dworkin RH, OConnor AB, Audette J, etal. Recommendations for the pharmacological management of neuropathic pain:an overview and literature
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6. Watson CP, Evans RJ, Reed K, etal. Amitriptyline versus placebo in postherpetic neuralgia. Neurology 982; 32:67673.
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Chapter4
Anticonvulsants
David Lussier
Mechanisms ofaction
The analgesic activity of most anticonvulsants results from a combination of
diverse actions on the central nervous system, all decreasing central sensitization. These include sodium channel blockade, calcium channel blockade, suppression of glutamate release, and action on N-methyl-D -aspartate (NMDA)
receptors[].
Gabapentinoids
Gabapentin and pregabalin are thought to exert their analgesic action
mostly via modulation of the 2- protein of the N-type calcium channel.
Gabapentin also acts on NMDA receptors, protein kinase C, and inflammatory cytokines [2]. Arecent placebo-controlled study suggests that pregabalin
reduces insular glutamatergic activity, which reduces the increased functional
connectivity seen in chronic pain; neuroimaging markers predict analgesic
response to pregabalin[3].
Gabapentin and pregabalin are both minimally bound to proteins and are
not metabolized by the liver, and they are thereby devoid of pharmacokinetic
drug-drug interactions. Pregabalin possesses a significant advantage over gabapentin, because it does not require active transporters to be absorbed, and
therefore it has linear pharmacokinetics, which makes dose titration easier and
allows twice-daily dosing [4]. Gabapentin, the saturable absorption process of
which makes its bioavailability lower at higher doses (35% for 600 mg three
21
21
Introduction
Anticonvulsants
Chapter4
22
times daily vs 60% for a single 300 mg dose), requires administration 34 times
daily [4]. However, the newer formulations of gastroretentive gabapentin and
gabapentin enacarbil allows a once- and twice-daily administration, respectively. Pregabalin has a faster onset of action than gabapentin [5].
Gabapentin greatly expanded the use of anticonvulsants in pain management, due to several studies supporting its efficacy and its better tolerability
than older anticonvulsants. Similarly to antidepressants, diabetic neuropathy
[6,7] and postherpetic neuralgia [8,9] are the neuropathic conditions for
which the analgesic efficacy of gabapentin has been the most studied, with
several randomized controlled trials (RCTs) supporting it. Its use in acute herpes zoster [0], spinal cord injury [], postthoracotomy pain [2], and lumbar spinal stenosis [3] is also supported by at least one RCT. Although limited
to open-label trials, evidence also suggests it might be effective to treat pain
from complex regional pain syndrome [4], human immunodeficiency virus
(HIV) neuropathy [5], and multiple sclerosis [6], as well as cancer-related
neuropathic pain (see Chapter9.2). As explained in Chapter9., comparative
trials of analgesics of different classes for the management of neuropathic
pain are very rare. When compared with amitriptyline, gabapentin was shown
to be either equally [7] or more effective [7]and better tolerated [7] to treat
diabetic neuropathy, whereas it was equally effective but better tolerated
than nortriptyline to treat postherpetic neuralgia [8]. Albeit limited, there
is some evidence that gabapentin might relieve pain from fibromyalgia[9].
Two new formulations of gabapentin have recently been introduced but
are not yet marketed in all countries. Agastroretentive formulation, the
pharmacokinetic properties of which allow daily administration of a 800 mg
dose, seems equally effective at similar doses, is better tolerated. and has a
shorter titration period than immediate-release gabapentin [20], with efficacy
and safety assessed for up to 24-week treatment [2]. Gabapentin enacarbil is an actively transported prodrug of gabapentin that provides sustained,
dose-proportional exposure to gabapentin, allowing a twice-daily administration. Relief of pain associated with postherpetic neuralgia seems to occur at
doses similar to gabapentin [22]. Evidence is supporting recommendation to
use gastroretentive gabapentin as first-line therapy for postherpetic neuralgia,
but it is still insufficient for gabapentin enacarbil[23].
Pregabalin, which possesses the same mechanism of action as gabapentin
with better pharmacokinetic properties, has also been extensively studied and
shown effective for diverse types of neuropathic pain, including painful diabetic
neuropathy [24,25] and postherpetic neuralgia [5]. Similarly to gabapentin,
pregabalin was shown effective to treat central pain from spinal cord injury [26].
More importantly, prolonged 5-month benefits have been shown for neuropathic pain refractory to other adjuvant (gabapentin, antidepressants) and opioid analgesics [27]. In a meta-analysis of 7 RCTs evaluating 7 oral medications
for chronic peripheral neuropathic pain and comprising close to 6000 subjects,
600 mg/day pregabalin had the largest beneficial effects along with 60 or 20
mg/day duloxetine [28]. Scientific data of its efficacy in fibromyalgia is sufficient
to make it a first-line recommended analgesic (see Chapter9.3). It can also
relieve pain from irritable bowel syndrome and has been used for chronic pancreatitis [29]. Compared with a twice-daily administration of 300 mg, a single
Anticonvulsants
Chapter4
23
24
Chapter4
Anticonvulsants
Table4. Mechanism of action, dosing recommandations, contraindications and adverse effects of anticonvulsants most
commonly used for pain management
Drug
Mechanism of Action
Starting Dose
Gabapentin
immediaterelease
00300 mg daily;
titrate by 00300
mg every one to
three days to an
effective dose
300 mg qd, titrate
up to 800 mg qd
over 5days
600 mg qd, titrate
to 600 mg bid
after 3days
2575 mg qd
00200 mg
qd-bid
Gastroretentive
gabapentin
Gabapentin
enacarbil
Pregabalin
Carbamazepine
Blockage of voltage-gated
sodium channels cell
excitability
Usual Effective
dose
300200 mg tid
800 mg qd
Precautions and
Contraindications
Decrease dose in patients with renal
dysfunction (avoid in severe renal
dysfunction).
Rapid discontinuation may result
in headache, nausea, insomnia, and
diarrhea.
Commonly Reported
Adverse Effects
Sedation, dizziness, tremor,
peripheral oedema, weight
gain, nausea, headache
600 mg bid
50300 mg bid
300800 mg bid
Oxcarbazepine2
Idem as carbamazepine
Dizziness
Lamotrigine
) Blockage of
voltage-gated sodium
channels cell
excitability
2) glutamatergic
neurotransmission via
glutamate receptors
3) GABAergic
neurotrasmission
25 mg qd; titrate
by 25 mg every
7days to an
effective dose
00200 mg bid
Topiramate
) Blockage of
voltage-gated sodium
channels cell
excitability
2) GABAergic
neurotrasmission
2550 mg qd;
00400 mg bid
titrate by 25 mg
every 57days to
an effective dose
25
Chapter4
Anticonvulsants
26
Chapter4
Anticonvulsants
Table4.Continued
Levetiracetam
Lacosamide
Zonisamide
250500 mg bid
Unknown. Possible blockade 50 mg bid
of voltage-gated sodium
channel
00 mg qd
500500 mg bid
Somnolence, dizziness
200400 mg bid
00300 mg bid
Pregabalin is better tolerated, and equally effective, with a single nightly dose rather than twice-dailydosing.
Anticonvulsants
Chapter4
Lamotrigine
Topiramate
Levetiracetam
Levetiracetam, which was once a promising agent due to animal and experimental data, good tolerability, and ease of dosing, has failed to show any
analgesic efficacy in several pain conditions, including central neuropathic
post-stroke pain [48], multiple sclerosis [49], and polyneuropathy[50].
Lacosamide
Lacosamide has been shown to be effective to treat neuropathic pain from
diabetic neuropathy, but with a very mild effect, and it has failed to show
benefits in fibromyalgia[5].
Zonisamide
Evidence for zonisamide is limited to one RCT in diabetic neuropathy[52].
Tiagabine
Evidence of analgesic efficacy for tiagabine is either anecdotal or limited to
open-label studies.
27
Individual randomized trials have shown that topiramate can relieve pain from
diabetic neuropathy [43], chronic low back pain [44], and chronic lumbar radicular pain [45], as well as improve anger, subjective disability, and health-related
quality of life in patients with low back pain [44]. Its analgesic effect might be
exerted via decreased peripheral nerve excitability [46]. However, available evidence has been deemed insufficient to support its use in neuropathic pain[47].
Anticonvulsants
Chapter4
Felbamate
Evidence of analgesic efficacy for felbamate is also either anecdotal or limited
to open-label studies.
Because of very limited evidence of analgesic efficacy, lacosamide,
zonisamide, tiagabine, and felbamate should only be considered as analgesics
after trials of other analgesics with better evidence of efficacy.
28
Conclusions
Anticonvulsants possess analgesic efficacy in a variety of painful conditions.
Evidence is best for neuropathic pain, for which pregabalin, gabapentin,
oxcarbazepine, lamotrigine, and topiramate have been shown to be effective, with much better evidence for the gabapentinoids. The latter also seem
to possess some analgesic efficacy for fibromyalgia and the management of
perioperative pain, including prevention of chronic postsurgical pain. With
all medications, one should always consider potential benefits, common and
serious adverse effects, as well as contraindications when considering prescribing an anticonvulsant as part of pharmacological management of pain,
and clinicians should favor those with the best efficacy/adverse effectsratio.
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26. Siddall PJ, Cousins MJ, Otte A, etal. Pregabalin in central neuropathic pain
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Chapter5
Cannabinoids
In several countries, such as Canada, and in some states in the United
States of America, the use of marihuana (marijuana, cannabis) is authorized
for medical purposes. However, cannabis remains illegal throughout the
United States and is not approved for prescription as medicine; however,
8 statesAlaska, Arizona, California, Colorado, Connecticut, Delaware,
Hawaii, Maine, Massachusetts, Michigan, Montana, Nevada, New Jersey,
New Mexico, Oregon, Rhode Island, Vermont, and Washington, as well
as the District of Columbiaapprove and regulate its medical use . The
Federal government continues to enforce its prohibition in these states. In
Canada, the seedlings are produced and delivered by Health Canada with a
special medical authorization. Marijuana inhalation exposes the user to many
chemical compounds including approximately 70 different phytocannabinoids
(9-tetrahydrocannabinol [9-THC], cannabinol, cannabidiol (CBD), cannabigerol, cannabichromene, tetrahydrocannabivarin, etc). In addition to the
whole plant, there are synthetic compounds available for prescription such as
9-THC or synthetic derivatives (Table 5.). The distributed dried marijuana
has a content of 2.5 2% 9-THC. Cannabinoid-based medicines have
been evaluated in several clinical trials for their potential role in the treatment
of different pain conditions. After a rapid presentation of the cannabinoid
system, the role of cannabinoids in various pain conditions is presented.
The cannabinoidsystem
Since the identification of the principal psychoactive component of cannabis,
many data suggest that the cannabinoid system is implicated in pain modulation via the activation of two cloned G-protein coupled receptors (Gi/o,
inhibiting type), cannabinoid receptor (CB) and CB2 receptors []. The CB
receptors are mainly localized in the central nervous system, and they are
also found along the pain pathways (primary afferent fibers and spinal cord).
By contrast, CB2 receptor expression seems to be found predominantly, but
not exclusively, in peripheral tissues with immune functions, although they
were also detected in the brain, dorsal root ganglia, lumbar spinal cord, on
sensory neurons, on microglia, and in peripheral tissues. Endogenous compounds such as anandamide and 2-arachidonoyl glycerol form the basis of the
endocannabinoid system (Figure 5.). Modulation of the endocannabinoid
http://medicalmarijuana.procon.org/view.resource.php?resourceID=00088 (accessed 25 March203)
33
33
34
Chapter5
Indications
Posology
Commercial
Name
Remarks
Marijuana
Plant
Individual
Dronabinol
2.5 to5mg
every2h
max. 20 mg/day
Marinol
In Canada,
requires a
special medical
authorization
from Health
Canada
Also used in
chronic pain
management
to2mg
every2h
max. 6 mg/day
Cesamet
Also used in
chronic pain
management
Oromucosal
spray containing
2.7 mg THC
and 2.5 mg
cannabidiol per
00L
Start with
sprayevery
4 h orless
Averagedose:
5 sprays/day
Sativex
Causes
irritations in
the mouth
in 2025%
patients in
clinical trials
Nabilone
Nabiximols
(THC/
cannabidiol)
Cannabinoids
CB1
CB2
Intracellular signalling
. G-protein activation
. Inhibition of AC
.Activation MAPK
.K+ channels
0
.Ca++ channels
0
Analgesia
Cannabinoids
Synthetic
?
.
Anti-inflammatory
Figure5. Schematic figure illustrating cannabinoid receptor (CB) and CB2 receptors and their agonists, and the endocannabinoid (endoCB)-mediated synaptic signaling
at glutamatergic synapses. Endocannabinoid signaling is a key regulator of neuronal
excitability and both excitatory and inhibitory synaptic transmission throughout the
central nervous system. It is regulated by synthesis, release, reuptake, and degradation
of endoCBs. ()Synthesis:endoCB signaling machinery operates on demand in a
synapse-specific manner, and endoCBs can be released immediately from postsynaptic
neurons. Enzymatic processes can be activated either by membrane depolarization,
increases in intracellular calcium levels, or receptor stimulation, leading to the cleavage of membrane phospholipid precursors and subsequent synthesis of endoCBs.
(2)Release:endoCBs can act through a retrograde signaling mechanism:released
from depolarized postsynaptic neurons into the extracellular space, they can travel to
presynaptic terminals, where they can activate cannabinoid receptors and downstream
signalization cascade leading to analgesic and anti-inflammatory effects. In this figure
illustrating a glutamatergic synapse, endoCBs can inhibit the release of the excitatory
neurotransmitter glutamate, thus temporarily inhibiting glutamatergic excitatory postsynaptic currents. (3)Reuptake of endoCBs, and most notably anandamide (AEA), in
the synaptic space have been recently shown to be facilitated by a specific transporter.
The existence of similar mechanisms for 2-arachidonoylglycerol (2-AG) transport
remains controversial. (4)Degradation:the synthesis and metabolism of AEA and
2-AG are controlled by distinct enzymatic pathways. Anandamide is hydrolyzed by
the enzyme fatty acid amide hydrolase (FAAH) in postsynaptic neurons, producing
ethanolamine and arachidonic acid, whereas 2-AG is degraded, predominantly but
not exclusively, by a distinct enzyme monoacylglycerol lipase (MGL) in presynaptic
neurons, generating glycerol and arachidonic acid. 9-THC, 9-tetrahydrocannabinol;
mGluR5, type metabotropic glutamate receptors.
35
Synthetic
Nabilone
Dronabinol
Nabiximols
.
Agonists:
Natural
9-THC
2-AG (CB2 > CB1)
(degraded by MAGL, FAAH)
Chapter5
Agonists:
Natural
9-THC
Anandamide(CB1 > CB2)
(degraded by FAAH)
Cannabinoids
Chapter5
36
system has been recently reviewed [2], indicating a significant role for the
endocannabinoid system in various pain conditions.
Acutepain
Cannabinoids have shown great efficacy in numerous animal models of acute
and inflammatory pain. However, they are least effective in alleviating acute
pain in human volunteers and in the postoperative setting. Indeed, in healthy
volunteers who were administered cannabinoids, only a few studies have demonstrated an analgesic effect [3,4]. Despite this negative outcome, it is important to note that in this setting of volunteer studies using noxious heat and
inflammatory stimuli, even potent and effective drugs such as opioids often
cannot achieve significant pain management [5]. Moreover, there are only four
published reports on the use of cannabinoids in postoperative pain, concluding
that cannabinoids administration is not appropriate to treat postoperative pain
and have either moderate effects [6,7], no effects different from placebo [8],
or even antianalgesic effects at high doses [9]. However, a large multicenter
study recruiting patients undergoing operations with a reproducible painful
condition and using appropriate dosage is needed before a conclusion can be
drawn on the effect of cannabinoids in acute postoperative pain management.
Chronicpain
In general, cannabinoids are moderately effective for the treatment of
chronic pain conditions [0]. Several recent studies using a substantial number of patients have shown that cannabinoids were effective in relieving pain in
patients suffering from several types of chronic pain, such as neuropathic pain
(including human immunodeficiency virus [HIV] neuropathic pain), spinal cord
injury (SCI), pain associated with multiple sclerosis (MS), musculoskeletal disorders, fibromyalgia, or other chronic pain conditions (for a review, see [,2]).
Neuropathicpain
Several randomized, placebo-controlled, double-blind, crossover and parallel
studies have evaluated cannabinoids for the relief of central or peripheral
neuropathic pain (see also Chapter9.). Overall, cannabinoids had modest
but significant analgesic effects often associated with adverse effects in the
treatment of neuropathic pain states. Patients suffering from neuropathic pain
of different etiologies reported benefits after treatment with 9-THC/CBD
concomitantly with other analgesic drugs [36]. However, negative outcomes were reported by two trials among neuropathic pain patients using
dronabinol and nabilone [7,8].
Numerous clinical trials have examined the efficacy of smoked cannabis for
neuropathic pain. For example, one randomized, placebo-controlled, crossover trial performed in 38 patients reported significant decreases in central and
peripheral neuropathic pain when using smoked cannabis [9]. More recently,
a randomized, placebo-controlled study evaluated smoked cannabis among
2 patients suffering from posttraumatic or postsurgical neuropathic pain
Cannabinoids
Spinal cordinjury
Although still limited, available clinical data support the findings of preclinical
animal studies [2527] suggesting that cannabinoids could alleviate symptoms
associated with neuropathic SCI such as pain, spasticity, muscle spasms, urinary
incontinence, and difficulty sleeping. Two double-blinded, placebo-controlled,
crossover studies performed in patients suffering from SCI suggested modest improvements in pain, spasticity, muscle spasms, and sleep quality with
oral 9-THC and/or 9-THC/CBD [3,28]. Arandomized, double-blind,
placebo-controlled parallel study using 9-THC showed a statistically significant improvement in spasticity scores in patients with SCI [29]. Moreover, a
recent double-blind, placebo-controlled, crossover study performed in 2
patients with SCI reported improved Asworth (spasticity) scores compared
with placebo after a treatment with nabilone (0.5 mg b.i.d.) for 4 weeks [30].
Although no definitive clinical conclusions can be made, these studies suggest a
potential benefit of cannabinoids in patients suffering fromSCI.
37
Multiple sclerosis
Preclinical studies and many clinical studies support cannabinoids use to alleviate symptoms associated with MS (reviewed in Ref. [3]). Accordingly, mostly
all clinical trials devoted to the use of cannabinoids in pain and spasticity treatment associated with MS were positive. For example, the Cannabis in Multiple
Sclerosis (CAMS) study, a large multicentre, randomized, placebo-controlled
trial, evaluated oral cannabis extracts 9-THC/CBD, oral 9-THC, or a placebo for 5 weeks in 630 patients suffering from MS. Subjective pain scores and
spasticity were significantly better in the cannabinoids group, but there was no
difference in the overall spasticity scores using the Ashworth scale [32]. Other
randomized clinical studies using cannabis extract 9-THC/CBD [33,34] and
Chapter5
Cannabinoids
Chapter5
38
standardized cannabis extract capsules [35] reported similar results, with subjective improvements of spasticity not confirmed by objective measures.
Nevertheless, a CAMS follow-up study showed a small long-term treatment effect of oral 9-THC on muscle spasticity measures by the Asworth
scale [36], and a long-term, open-label, follow-up study using 9-THC/CBD
concluded that positive effects were maintained in patients who had initially
perceived benefits [37]. Two other studies (a randomized, double-blind,
placebo-controlled, parallel-group trial and its extension) performed in
patients suffering from central neuropathic pain associated with MS revealed
that the oromucosal cannabis extract 9-THC/CBD was effective in reducing pain and sleep disturbances with a good adverse effects profile [38,39].
Moreover, a randomized, double-blind, placebo-controlled, crossover trial
concluded that an administration of 0 mg of dronabinol had a modest but
clinically relevant analgesic effect on central pain in patients with MS, with a
pain reduction similar to traditional analgesics [40]. Overall, although results
seem to be clinically significant mostly on subjective measures, cannabinoids
may be effective to relieve MS associated pain (for a review, see Ref.[4]).
Musculoskeletalpain
Cannabinoids may have a role in the alleviation of symptoms associated with
rheumatoid arthritis, as suggested by the identification of a functional endocannabinoid system in the knee synovia of patients suffering from end-stage
osteoarthritis and rheumatoid arthritis [42] (see also Chapter9.3). Arandomized, double-blinded, placebo-controlled, multicentre parallel group
study performed in 58 patients suffering from rheumatoid arthritis indicated
that a 9-THC/CBD extract administered for five weeks was a modest but
statistically significant analgesic for pain on movement and at rest, and it also
exerted benefits on quality of sleep with outcomes favoring cannabis over
placebo [43]. Another study involving patients suffering from refractory musculoskeletal pain [44] showed that nabilone had significant analgesic effects
compared with placebo. However, according to a recent review, there is
currently weak evidence that oromucosal cannabis is superior to placebo in
reducing pain in patients suffering from rheumatoid arthritis[45].
Fibromyalgia
In some diseases, cannabinoids might be effective in only a subpopulation of
patients suffering from that disease. For example, an open-label pilot study
performed in patients suffering from fibromyalgia examined the effect of
dronabinol on experimentally induced pain, axon reflex flare, and pain relief
and reported that only some patients experienced significant pain relief, with
a high dose [46]. However, intolerable adverse effects caused a high rate of
patient dropout. Arandomized, double-blind, placebo-controlled trial was
performed in 40 patients suffering from fibromyalgia [47] with nabilone mg
b.i.d. for four consecutive weeks. Patients subjectively reported significant
improvements in pain relief and anxiety, as well as in Fibromyalgia Impact
Questionnaire scores. However, nabilone treatment did not attenuate the
number of tender points nor the tender point pain threshold, and it did not
retain any lasting benefit after its discontinuation. Amulticenter retrospective
Cannabinoids
Chapter5
Four studies performed more than 34years ago have valued cannabinoids
potential for cancer-related pain treatment. The first two studies are randomized, double-blind, placebo-controlled trials evaluating the analgesic effectiveness of oral 9-THC (dronabinol) in patients suffering from moderate to
severe refractory cancer pain. The first study was performed in 0 cancer
patients treated with an escalating dose of 5, 0, 5, and 20 mg 9-THC
[50]. Patients reported significant pain relief with the two higher doses but
unfortunately also experienced severe adverse effects. The second study
was performed in 36 cancer patients comparing 0 and 20 mg 9-THC with
60 and 20 mg of codeine [5]. Patients reported mild analgesic effects, but
9-THC highest dose induced somnolence, dizziness, ataxia, and blurred
vision. However, authors concluded that a 0 mg 9-THC regimen, despite
its sedative effect, seemed to have analgesic potential in these patients.
Adverse effects apparently interfered with cannabinoids benefits in this context. Indeed, another study tested a nitrogen analog of 9-THC in cancer
patients and reported that although pain relief was superior to placebo and
approximately equivalent to 50 mg of codeine phosphate, the synthetic analog was not considered clinically useful because of the adverse effects profile
[52]. In contrast, a study comparing a 9-THC nitrogen analog with codeine
and placebo in patients suffering from chronic pain due to malignancies demonstrated that benzopyranoperidine (a synthetic analog of 9-THC) did not
produce analgesic effects and even seemed to increase pain perception[53].
A recent randomized, double-blinded, placebo-controlled, parallel-group
study evaluated a cannabis extract (9-THC/CBD), a 9-THC extract, and
placebo in 77 patients suffering from intractable cancer-associated pain not
fully relieved by strong opioids [54]. Approximately 43% of patients subjectively reported a 30% or greater improvement in pain score, which was twice
the number of patients who achieved this response in the 9-THC and placebo groups. Both cannabinoid regimens were well tolerated, and adverse
effects were mild to moderate (somnolence, dizziness, and nausea).
Additional clinical trials evaluating the therapeutic efficacy of cannabinoids
in cancer pain are needed, especially given cannabinoids additional therapeutic potential regarding antiemetic and antitumour properties (for a review,
see Ref.[55]).
39
Cancerpain
Cannabinoids
Chapter5
40
Opioids-cannabinoids interactions
Because cannabinoids and opioids are distinct drug classes with different
effects on pain modulation and pain-relieving mechanisms, there has been
considerable clinical interest in investigating combinations of different opioids
and cannabinoids to enhance the potency of both compounds.
Some clinical reports support the use of combined administration of
cannabinoids and opioids for peripheral inflammatory pain, acute pain, and
chronic pain in human volunteers. In addition, a study has examined the effect
of adding a cannabinoid to the regimen of patients experiencing chronic pain
despite taking stable doses of opioids and has concluded that dronabinol
may be a useful adjuvant analgesic for these patients (for a review, see Ref.
[58]). Moreover, a recent clinical trial was performed in 2 patients suffering from chronic pain using inhaled vaporized cannabis concomitantly with
sustained-release morphine or oxycodone. The authors concluded that cannabis augments analgesia in patients already on a stable opioid regimen without significantly altering plasma opioid levels or metabolism[59].
Overall, opioid and cannabinoid interactions may lead to additive or even
synergistic antinociceptive effects, emphasizing their clinical relevance in
humans in order to reduce requirements for opioids.
Conclusions on cannabinoids as
adjuvant analgesics
Although preclinical evidence highlights the importance of cannabinoid receptors in controlling nociceptive transmission, data obtained from clinical trials are less conclusive regarding the analgesic efficacy of smoked marijuana
and synthetic cannabinoids [60, 6]. In acute pain trials, negative or equivocal
Cannabinoids
Chapter5
Central NervousSystem
Euphoria, dysphoria
Anxiety/nervousness
Amnesia, confusion, depersonalization
Drowsiness, dizziness, somnolence
Transient impairment of sensory and perceptual functions
Psychomotor retardation
Cognitive impairments
Depression, amotivational syndrome, psychosis, schizophrenia
RespiratoryTract
Decreased pulmonary function
Chronic obstructive airway diseases
Pulmonary infections
ImmuneSystem
Immunomodulatory/immunosuppressive effects
Reproductive and EndocrineSystem
Reduced neonatal birth weight andlength
Slightly increased risk of sudden infantdeath
Decline in sperm count, concentration and motility
Increase in abnormal sperm morphology
CardiovascularSystem
Dose-related tachycardia
Fluctuations in blood pressure
Coronary insufficiency
Myocardial infarction
Peripheral vasodilation, postural hypotension, and characteristic conjunctival
reddening
Liver
Implication in chronic liver diseases
Association with moderate to severe fibrosis
Carcinogenesis and Mutagenesis
Mutagenic effects
Precancerous pulmonary pathology
Tolerance, Dependence andAbuse
Dependence in out of 0people
Behaviors of preoccupation, compulsion, reinforcement, and withdrawal
Overdose/Toxicity
No documented evidence of death directly attributable to cannabis overdose
41
Cannabinoids
Chapter5
42
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Pain:IASP Press, Seattle; 200:pp. 38.
2. Guindon J, Hohmann AG. The endocannabinoid system and pain. CNS Neurol
Disord Drug Targets 2009; 8:40342.
3. Redmond WJ, Goffaux P, Potvin S, et al. Analgesic and antihyperalgesic
effects of nabilone on experimental heat pain. Curr Med Res Opin 2008;
24:07024.
4. Rukwied R, Watkinson A, McGlone F, etal. Cannabinoid agonists attenuate
capsaicin-induced responses in human skin. Pain 2003; 02:283288.
5. Naef M, Curatolo M, Petersen-Felix S, et al. The analgesic effect of oral
delta-9-tetrahydrocannabinol (THC), morphine, and a THC-morphine combination in healthy subjects under experimental pain conditions. Pain 2003;
05:7988.
6. Jain AK, Ryan JR, McMahon FG, etal. Evaluation of intramuscular levonantradol and placebo in acute postoperative pain. J Clin Pharmacol 98; 2(89
Suppl):320S326S.
7. Holdcroft A, Maze M, Dore C, et al. A multicenter dose-escalation
study of the analgesic and adverse effects of an oral cannabis extract
(Cannador) for postoperative pain management. Anesthesiology 2006;
04:040046.
8. Buggy DJ, Toogood L, Maric S, et al. Lack of analgesic efficacy of
oral delta-9-tetrahydrocannabinol in postoperative pain. Pain 2003;
06:6972.
9. Beaulieu P. Effects of nabilone, a synthetic cannabinoid, on postoperative pain.
Can J Anaesth 2006; 53:769775.
0. Beaulieu P, Ware M. Reassessment of the role of cannabinoids in the management of pain. Curr Opin Anaesthesiol 2007; 20:473477.
. Martin-Sanchez E, Furukawa TA, Taylor J, et al. Systematic review and
meta-analysis of cannabis treatment for chronic pain. Pain Med 2009;
0:353368.
2. Lynch ME, Campbell F. Cannabinoids for treatment of chronic non-cancer
pain; a systematic review of randomized trials. Br J Clin Pharmacol 20;
72:735744.
Cannabinoids
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3. Wade DT, Robson P, House H, etal. A preliminary controlled study to determine whether whole-plant cannabis extracts can improve intractable neurogenic symptoms. Clin Rehabil 2003; 7:229.
4. Berman JS, Symonds C, Birch R. Efficacy of two cannabis based medicinal
extracts for relief of central neuropathic pain from brachial plexus avulsion:results of a randomised controlled trial. Pain 2004; 2:299306.
5. Notcutt W, Price M, Miller R, etal. Initial experiences with medicinal extracts
of cannabis for chronic pain:results from 34N of studies. Anaesthesia
2004; 59:440452.
6. Nurmikko TJ, Serpell MG, Hoggart B, etal. Sativex successfully treats neuropathic pain characterised by allodynia: a randomised, double-blind,
placebo-controlled clinical trial. Pain 2007; 33:20220.
7. Attal N, Brasseur L, Guirimand D, etal. Are oral cannabinoids safe and effective in refractory neuropathic pain? Eur J Pain 2004; 8:7377.
8. Frank B, Serpell MG, Hughes J, etal. Comparison of analgesic effects and
patient tolerability of nabilone and dihydrocodeine for chronic neuropathic
pain:randomised, crossover, double blind study. BMJ 2008; 336:9920.
9. Wilsey B, Marcotte T, Tsodikov A, etal. A randomized, placebo-controlled,
crossover trial of cannabis cigarettes in neuropathic pain. J Pain 2008; 9:50652.
20. Ware MA, Wang T, Shapiro S, etal. Smoked cannabis for chronic neuropathic
pain:a randomized controlled trial. CMAJ 200; 82:E694E70.
2. Abrams DI, Jay CA, Shade SB, etal. Cannabis in painful HIV-associated sensory neuropathy:a randomized placebo-controlled trial. Neurology 2007;
68:5552.
22. Ellis RJ, Toperoff W, Vaida F, etal. Smoked medicinal cannabis for neuropathic
pain in HIV:a randomized, crossover clinical trial. Neuropsychopharmacology
2009; 34:672680.
23. Ware MA. Clearing the smoke around medical marijuana. Clin Pharmacol
Ther 20; 90:76977.
24. Kalant H. Smoked marijuana as medicine:not much future. Clin Pharmacol
Ther 2008; 83:5759.
25. Hama A, Sagen J. Antinociceptive effect of cannabinoid agonist WIN 55,22-2
in rats with a spinal cord injury. Exp Neurol 2007; 204:454457.
26. Hama A, Sagen J. Sustained antinociceptive effect of cannabinoid receptor
agonist WIN 55,22-2 over time in rat model of neuropathic spinal cord injury
pain. J Rehabil Res Dev 2009; 46:3543.
27. Garcia-Ovejero D, Arevalo-Martin A, Petrosino S, etal. The endocannabinoid
system is modulated in response to spinal cord injury in rats. Neurobiol Dis
2009; 33:577.
28. Maurer M, Henn V, Dittrich A, etal. Delta-9-tetrahydrocannabinol shows
antispastic and analgesic effects in a single case double-blind trial. Eur Arch
Psychiatry Clin Neurosci 990; 240:4.
29. Hagenbach U, Luz S, Ghafoor N, et al. The treatment of spasticity with
Delta9-tetrahydrocannabinol in persons with spinal cord injury. Spinal Cord
2007; 45:55562.
30. Pooyania S, Ethans K, Szturm T, etal. A randomized, double-blinded, crossover pilot study assessing the effect of nabilone on spasticity in persons with
spinal cord injury. Arch Phys Med Rehabil 200; 9:703707.
3. Pertwee RG. Cannabinoids and multiple sclerosis. Mol Neurobiol 2007;
36:4559.
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44
Cannabinoids
Chapter5
45
49. Fiz J, Duran M, Capella D, etal. Cannabis use in patients with fibromyalgia:effect on symptoms relief and health-related quality of life. PLoS One
20; 6:e8440.
50. Noyes R Jr, Brunk SF, Baram DA, et al. Analgesic effect of
delta-9-tetrahydrocannabinol. J Clin Pharmacol 975; 5:3943.
5. Noyes R Jr, Brunk SF, Avery DA, et al. The analgesic properties of
delta-9-tetrahydrocannabinol and codeine. Clin Pharmacol Ther 975;
8:8489.
52. Staquet M, Gantt C, Machin D. Effect of a nitrogen analog of tetrahydrocannabinol on cancer pain. Clin Pharmacol Ther 978; 23:39740.
53. Jochimsen PR, Lawton RL, VerSteeg K, etal. Effect of benzopyranoperidine, a
delta-9-THC congener, on pain. Clin Pharmacol Ther 978; 24:223227.
54. Johnson JR, Burnell-Nugent M, Lossignol D, etal. Multicenter, double-blind,
randomized, placebo-controlled, parallel-group study of the efficacy, safety,
and tolerability of THC:CBD extract and THC extract in patients with intractable cancer-related pain. J Pain Symptom Manage 200; 39:6779.
55. Guindon J, Hohmann AG. The endocannabinoid system and cancer:therapeutic implication. Br J Pharmacol 20; 63:447463.
56. Lichtman AH, Martin BR. Cannabinoid tolerance and dependence. Handb Exp
Pharmacol 2005; 6977.
57. Wang T, Collet JP, Shapiro S, etal. Adverse effects of medical cannabinoids:a
systematic review. CMAJ 2008; 78:669678.
58. Desroches J, Beaulieu P. Opioids and cannabinoids interactions:involvement
in pain management. Curr Drug Targets 200; :462473.
59. Abrams DI, Couey P, Shade SB, et al. Cannabinoid-opioid interaction in
chronic pain. Clin Pharmacol Ther 20; 90:84485.
60. Hosking RD, Zajicek JP. Therapeutic potential of cannabis in pain medicine. Br
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7:388.
Chapter6
Local Anesthetics
Local anesthetics constitute a group of pharmacological agents that are
injected into the vicinity of a peripheral nerve or spinal cord. Local and
regional anesthesia is widely accepted as being a safe and even beneficial anesthetic technique for pain therapy with a low rate of complications []. Clinical
use of local anesthetics therefore requires basic knowledge of the anatomy
and physiology of peripheral and central pain transmission [2], technical skills
in localizing peripheral nerves and in the performance of nerve blocks [3], as
well as knowledge of the pharmacologic properties of these drugs [4]. Apart
from complications resulting from technical difficulties in performing the
nerve block, severe toxic complications result from inadvertent drug effects.
With the advent of ultrasound-guided regional anesthetic techniques [5] and
lipid rescue therapy [6], the application of local anesthetics has never been
as safe. Ultrasound imaging allows the precise injection of local anesthetics
directly into the vicinity of peripheral nerves under visual control. This technique helps to reduce the dose of the local anesthetic. Furthermore, physical
damage of nerves by the injection needle and inadvertent injection of local
anesthetics into blood vessels can also be decreased. Local anesthetics can
also be administered systemically or topically for some indications. Treatment
protocols have been developed for this clinical use. This chapter offers a
pharmacological and neurophysiological approach to the clinical use of a very
potent group of extremely beneficial pharmacological agents.
47
47
Patrick Friederich
Local Anesthetics
Chapter6
Incision blocks
Intra-articular and bursa blocks
Neuraxial blocks
48
Other blocks
Ophthalmic, otologic:drops
Cutaneous:creams (eutectic mixture of
local anesthetics), patch, gels, dentalpaste
Mucosa:vaporisation (buccal, pharyngeal,
bronchial, gastric, anal, etc)
Subcutaneous, subfascial
Epidural
Rachianesthesia
Caudal block
Plexus blocks:brachial, lumbosacral
Proximal and distal nerve blocks:face,
extremities
Intercostalblocks
Block of abdominal transverse or transversus
abdominis plane block
Rectus abdominisblock
Pectoral block
Dorsal penile nerveblock
Paravertebral block
Nociception
The primary afferent neurons involved in pain transmission are called nociceptors. They are activated by noxious stimuli such as mechanical, thermal,
or chemical insult threatening tissue integrity. Activation of nociceptors initiates nociception, that is, the transmission of neural information via peripheral
nerves and the spinal cord to the brain where this information is interpreted
as pain. Infiltration of local anesthetics into human tissue such as the skin aims
at preventing pain sensation by blocking activation of nociceptors and blockade of very superficially located peripheral endings of the primary afferent
neurons. Infiltration of local anesthetics into the skin or superficial tissue only
makes sense if the region of insult is restricted to a very small superficial anatomical region. If nociceptive information is transmitted from larger regions
than a small and defined local area, a peripheral nerve block or neuraxial analgesia that covers a larger region of the body needs to be considered[3].
Transmission of nociceptive information by
peripheralnerves
Peripheral nerves transmit information from peripheral regions of the human
body to the brain. The more distal the nerve is from the brain, the smaller
is the anatomic region it transmits information from. The peripheral nerves
most frequently blocked by local anesthetics clinically derive from either the
brachial plexus or the lumbosacral plexus. Peripheral nerves such as the radial
and ulnar nerves or the femoral and the sciatic nerves transmit sensation
from the upper and lower extremities, respectively [3]. They are blocked for
Local Anesthetics
Chapter6
49
surgeries on larger parts of a single upper or lower extremity such as surgeries for a fractured arm or leg. If the region of interest is too large for a single
or a limited number of nerve blocks, the entire plexus may be approached for
blockade by local anesthetics.
Nociceptive information originating in the thoracic region is transmitted by
intercostal and subcostal nerves via the dorsal and ventral rami of the spinal
nerves to the spinal cord. The muscles and skin of the back of the body are
supplied by the dorsal rami of the spinal nerves. Intercostal and subcostal
nerves can easily be blocked by local anesthetics. Such blocks may be performed for treatment of postherpetic neuralgia or for alleviating pain resulting
from thoracotomy or rib fracture.
Local Anesthetics
Chapter6
50
Local Anesthetics
Chapter6
51
Local Anesthetics
Chapter6
52
Esters
Procaine
Chloroprocaine
Tetracaine
Amides
Lidocaine
Prilocaine
Mepivacaine
Bupivacaine
Levobupivacaine
Etidocaine
Ropivacaine
Duration
of Action
(h)
Potency
236
27
264
8.9
8.7
8.5
6
?
80
Long
Short
Long
.5
0.5
34
0.5
234
220
246
288
288
276
274
7.9
7.6
7.6
8.
8.
7.7
8.
65
55
75
95
95
95
94
Short
Short
Short
Intermediate
Intermediate
Short
Intermediate
.52
.52
23
33.5
33.5
34
2.53
4
4
4
3.3
Local Anesthetics
Chapter6
As a clinically applicable rule of thumb, it seems fair to assume that the higher
the hydrophobicity or the higher the octanol-buffer coefficient, the slower
the onset; however, the higher the potency, the longer the duration of effect,
but also the higher the risk of severe side effects after inadvertent systemic
application (Figure 6.). Local anesthetics with a short or medium duration
of action (such as lidocaine or mepivacaine) have a relatively wide therapeutic margin even allowing, as in the case of lidocaine, intravenous application.
However, long-acting local anesthetics without the potential to induce severe
side effects have yet to be developed for clinical application. Whether this will
be achieved by alternative pharmacological strategies remains an important
area of research [4,5].
The potency of local anesthetic interaction with many different cellular structures such as ion channels correlates with their octanol-buffer
coefficient [6,7]. The most famous explanation for this relationship is
provided by the guarded receptor hypothesis (Figure 6.2). This hypothesis
[8] states that local anesthetics are capable of suppressing cardiac action
potentials by blocking sodium channels following drug binding to a partially
hydrophobic site on the channel when they are open. The drug molecules
disappear from the sodium channel when they are closed. However, the
time constant for disappearance or unblock is determined by the hydrophobicity. The more hydrophobic the drug is, the slower this drug disappears from the receptor and hence the longer the duration of action. This
result usually is desirable for the blockade of pain transmission in peripheral nerves. However, it is entirely undesirable at other parts of the body
such as the central nervous system or the heart, where blockade of ion
channels and other molecular structures [9] may cause severe arrhythmia
and sudden cardiac death[20].
From a therapeutic point of view, severe side effects of local anesthetics can
be divided into two classes:class Aand class B side effects. Class Aside effects
result from inadvertent systemic application of the drug that results in direct
drug effects on the brain or the cardiovascular system. This usually happens
in drug-induced seizure and cardiac arrhythmia. Class Aside effects are most
dangerous when resulting from long-acting local anesthetics such as bupivacaine;
therapy is then extremely challenging and needs to be installed quickly. However,
with the advent of lipid rescue therapy, the situation has changed considerably
and successful treatment of severe intoxication has become easier[6].
Class B side effects results from direct toxic drug effects on central and
peripheral nerves that result in transient radicular irritation, peripheral neuropathies, or cauda equina syndrome. These underlying toxic mechanisms
include induction of inflammation and apoptosis of nerve cells [2,22]. To
some extent, class B side effects depend on the choice of drug (lidocaine
5%) and the regional anesthetic technique (spinal anesthesia) [23]. These side
effects may last from days to persistent nerve damage without therapeutic
options if they result from direct drug effects. To reduce the risk for these side
53
54
Chapter6
Time [ms]
0 100 200 300 400 500 600 700 800 900 100011001200130014001500160017001800
40
Potential [mV]
ventricular
actionpotential
20
0
2
40
60
80
sodium
current
Potential [mV]
100
50
50
100
150
200
250
300
350
block
Inhibition
0.5
R
Bupivacaine
Ropivacaine
Lidocaine
Figure6.2 According to the guarded receptor hypothesis, local anesthetics block sodium currents during systole and dissociate from the
ion channels during diastole. The time constant for disappearance is determined by the hydrophobicity. The more hydrophobic the drug,
the slower this drug disappears from the channel and the higher the risk of cumulative block and cardiac arrhythmia. Experimental data on
ropivacaine are limited. I, inactivated channel; O, open channel; R, resting channel.
Local Anesthetics
3 mg/kg
4.5 mg/kg (7 mg/kg if used with epinephrine/adrenaline)
8 mg/kg
3 mg/kg
3 mg/kg
3 mg/kg
Local Anesthetics
Chapter6
55
effects, the maximum daily dose of local anesthetic should not be exceeded.
When various local anesthetics are used, the doses are additive (Table6.3).
Several epidemiologic studies [24,25] report incidences of nerve injury
such as transient radicular irritation, cauda equina syndrome, as well as
peripheral neuropathies ranging from in 8000 to in 6.Due to their specific interactions with cardiac ion channels, local anesthetics are capable of
inducing severe arrhythmias and cardiac arrest. Although the overall incidence of toxic complications seems low, local anesthetic-induced toxicity
is not evenly distributed among different regional anesthetic techniques. In
adult patients, major nerve blocks requiring large doses of local anesthetics are associated with a seizure incidence of up to 2 in 000. Although
no such complication was observed in caudal anesthesia, the incidence of
cardiac arrest is 6 times higher ( in 600)in spinal anesthesia than in epidural anesthesia or major nerve block. Transient radicular irritation occurs
more frequently than any other toxic side effect of local anesthetics with a
reported incidence of up to 30%. Fortunately, neurotoxic side effects causing longer-term neurologic impairment such as cauda equina syndrome are
rare, occurring in in 0 000 patients. In a recent study []on the incidence of local anesthetic systemic toxicity and postoperative neurologic
symptoms resulting from ultrasound-guided peripheral regional anesthetic
techniques, the incidence was .8% for postoperative neurologic symptoms
lasting longer than 5days and 0.9 for postoperative neurologic symptoms
lasting longer than 6months. The incidence for seizure was below 0.%, and
cardiac arrests were not observed in the study population of more than
2 600 patients.
Clinical signs of local anesthetics toxicity are mostly cardiovascular and
neurological (Table 6.4). Allergic reactions are rare after administration of
a local anesthetic, but local anesthetics solutions can contain conservation
agents, such as methylparabene, which can cause allergic reactions.
Local Anesthetics
Chapter6
56
References
. Sites BD, Taenzer AH, Herrick MD, etal. Incidence of local anesthetic systemic toxicity and postoperative neurologic symptoms associated with 2,668
ultrasound-guided nerve blocks:an analysis from a prospective clinical registry.
Reg Anesth Pain Med 202; 37:478482.
2. Yaksh TL, Luo ZD. Anatomy of the pain processing system. In:Waldman SD
ed, Pain Management. st ed. Philadelphia, PA:Saunders; 2007:pp.20.
3. Wedel DJ, Horlocker TT. Nerve blocks. In:Miller R, ed. Millers Anesthesia.
7th ed. Philadelphia, PA:Churchill Livingstone; 200:pp. 639674.
4. Berde CB, Strichartz GR. Local anesthetics. In:Miller R, ed. Millers Anesthesia.
7th ed. Philadelphia, PA:Churchill Livingstone; 200:pp. 93939.
5. Gray A. Ultrasound guidance for regional anesthesia. In:Miller R, ed. Millers
Anesthesia. 7th ed. Philadelphia, PA:Churchill Livingstone; 200:pp. 675704.
6. Weinberg GL. Lipid emulsion infusion:resuscitation for local anesthetic and
other drug overdose. Anesthesiology 202; 7:8087.
7. Herroeder S, Pecher S, Schnherr ME, et al. Systemic lidocaine shortens
length of hospital stay after colorectal surgery:a double-blinded, randomized,
placebo-controlled trial. Ann Surg 2007; 246:92200.
26. Auroy Y, Benhamou D, Bargues L, etal. Major complications of regional anesthesia in France:The SOS Regional Anesthesia Hotline Service. Anesthesiology
2002; 97:274280.
Local Anesthetics
Chapter6
57
8. Marret E, Rolin M, Beaussier M, Bonnet F. Meta-analysis of intravenous lidocaine and postoperative recovery after abdominal surgery. Br J Surg 2008;
95:33338.
9. De Oliveira GS Jr, Fitzgerald P, Streicher LF, et al. Systemic lidocaine to
improve postoperative quality of recovery after ambulatory laparoscopic surgery. Anesth Analg 202; 5:262267.
0. Chen WK, Miao CH. The effect of anesthetic technique on survival in human
cancers:a meta-analysis of retrospective and prospective studies. PLoS One
203; 8:e56540.
. Piegeler T, Votta-Velis EG, Liu G, etal. Antimetastatic potential of amide-linked
local anesthetics:inhibition of lung adenocarcinoma cell migration and inflammatory Src signaling independent of sodium channel blockade. Anesthesiology
202; 7:548559.
2. Stow PJ, Glynn CJ, Minor B. EMLA cream in the treatment of post herpetic
neuralgia:efficacy and pharmacokinetic profile. Pain 989; 39:30305.
3. Attal N, Cruccu G, Baron R, etal. EFNS guidelines on the pharmacological
treatment of neuropathic pain:200 revision. Eur J Neurol 200; 7:3-e88.
4. Polley LS, Columb MO. Ropivacaine and bupivacaine:concentrating on dosing!
Anesth Analg 2003; 96:25253.
5. Kohane DS, Smith SE, Louis DN, etal. Prolonged duration local anesthesia from tetrodotoxin-enhanced local anesthetic microspheres. Pain 2003;
04:4542.
6. Weiniger CF, Golovanevski L, Domb AJ, Ickowicz D. Extended release formulations for local anaesthetic agents. Anaesthesia 202; 67:90696.
7. Punke MA, Friederich P. Lipophilic and stereospecific interactions of
amino-amide local anesthetics with human Kv. channels. Anesthesiology
2008; 09:895904.
8. Siebrands CC, Friederich P. Structural requirements of human ether-ago-go-related gene channels for block by bupivacaine. Anesthesiology 2007;
06:52353.
9. Clarkson CW, Hondeghem LM. Mechanism for bupivacaine depression of cardiac conduction: fast block of sodium channels during the action potential with
slow recovery from block during diastole. Anesthesiology 985; 62:396405.
20. Butterworth JF 4th. Models and mechanisms of local anesthetic cardiac toxicity:a review. Reg Anesth Pain Med 200; 35:6776.
2. Albright GA. Cardiac arrest following regional anesthesia with etidocaine or
bupivacaine. Anesthesiology 979; 5:285287.
22. Friederich P, Schmitz TP. Lidocaine-induced cell death in a human model of
neuronal apoptosis. Eur J Anaesthesiol 2002; 9:564570.
23. Werdehausen R, Fazeli S, Braun S, etal. Apoptosis induction by different local
anaesthetics in a neuroblastoma cell line. Br J Anaesth 2009; 03:778.
24. Zaric D, Pace NL. Transient neurologic symptoms (TNS) following spinal
anaesthesia with lidocaine versus other local anaesthetics. Cochrane Database
Syst Rev 2009 Apr 5;(2):CD003006.
25. Auroy Y, Narchi P, Messiah A, etal. Serious complications related to regional
anesthesia:results of a prospective survey in France. Anesthesiology 997;
87:479486.
Chapter 7
N-Methyl-D -aspartate
Antagonists
N-Methyl-D -aspartate (NMDA) receptor antagonists have been used in the
field of perioperative pain management not for their direct analgesic effects but
for their ability to reduce postoperative central pain sensitization and its clinical symptoms such as hyperalgesia, allodynia, and the development of chronic
postsurgical pain. The use of NMDA receptor antagonists for chronic neuropathic pain has been less studied. Nevertheless, in this chapter, we will review
their effect on both acute postoperative pain and chronic pain conditions.
To better understand the role of NMDA receptor antagonists and to
introduce what is expected from their use in the clinical setting, it is important to define the clinical signs of pain hypersensitivity, namely allodynia and
hyperalgesia.
59
59
N-Methyl-D-aspartate Antagonists
Chapter 7
60
N-Methyl-D-aspartate Antagonists
Ketamine
Ketamine is an NMDA-receptor antagonist. It blocks this receptor channel by
acting on a specific subunit of the receptor. Plasma concentration of ketamine
at 30 ng/mL seems to be sufficient to achieve a minimal analgesic effect [19]
and to obtain a decrease in pain and opioid consumption after surgery [20, 21].
CHAPTER 7
Opioid
receptors
PKC
Ca++
Tissue
Trauma
+
NMDA
receptors
+
Pain Inhibitory
Systems
Pain Facilitatory
Systems
+
NOCICEPTION
= ANALGESIA
= HYPERALGESIA
Figure 7. The graphic illustrates the link between -opioid receptors and
N-methyl-D-aspartate (NMDA) receptors. By activating a specific protein kinase C
, opioids have the ability to modulate or enhance the activity of NMDA receptors.
This might lead to an exaggeration of postoperative hyperalgesia. Adapted from
[16] with permission of Wolters Kluwer.
61
Opioids
N-Methyl-D-aspartate Antagonists
CHAPTER 7
62
Administered during and after surgery, ketamine has been shown to reduce
hyperalgesia when tested around the surgical wound [2, 22, 23].
Several recent meta-analyses demonstrated that the beneficial effect of
ketamine on postoperative pain and opioid consumption was lasting beyond
the elimination half-life of the drug [2429]. These findings suggest that ketamine possesses a longer lasting effect than its own pharmacologic effect to
block pain sensitization processes after surgery. As a consequence, ketamine
demonstrated long-lasting effects on the development of long-term pain sensitization. The most recent meta-analysis to date indicated that a large majority of clinical trials favor the use of perioperative ketamine for acute pain
management [27].
There is considerable variability of the ketamine regimens used in the literature to obtain an anti-hyperalgesic effect and to reduce acute postoperative pain and opioid requirements. Table 7. presents regimens that appear
to be practical and relevant [27, 30]. Intra- and postoperative intravenous
(i.v.) low doses of ketamine were also shown to reduce the development of
chronic pain at 6 months or 2 months after laparotomies [3, 8, 31].
Finally, the epidural administration of ketamine was reported to effectively
block pain sensitization [32]. However, this is not a recommended mode of
usage, due to the possible neurotoxic effect of the various solutions used in
different countries.
Other authors also reported on the use of S-ketamine. Regular ketamine
is a racemic mixture of S(+) ketamine and R() ketamine. However, S(+)
ketamine alone is now available in some countries. Its NMDA receptor affinity is four times greater than that of R() ketamine, and the analgesic effect is
said to be 23 times greater than the racemic presentation of the drug. More
clinical studies are needed to understand the role that S(+) ketamine will play
in perioperative pain management.
Ketamine
Maintenance
Postoperative
Repeated
boluses (stop
bolusing
30min
before end
ofsurgery)
Continuous
infusion
0.25 mg/kg
0.25 mg/kg
every 30 min
High Level
ofPain
0.5 mg/kg
0.25 mg/kg every
30 min
N-Methyl-D-aspartate Antagonists
CHAPTER 7
63
N-Methyl-D-aspartate Antagonists
CHAPTER 7
64
with some reporting positive results of i.v. magnesium to improve postoperative pain management [4446], and others failing to support its use [47
49]. This lack of effect of i.v. magnesium might be explained by the poor
crossing of the blood-brain barrier, as mentioned above. Nevertheless, a
recent meta-analysis reported that i.v. magnesium given perioperatively
could decrease the overall 24 hour morphine consumption by 24.4% and,
to a lesser extent, postoperative pain intensity (4.2 at rest, 9.2 on movement on a scale of 00) [50]. In most studies, magnesium is administered
as an i.v. bolus of 3050 mg/kg at the time of anesthesia induction, and it
is continued intra- and postoperatively with an average of 500 mg/h for
24 hours [50].
When given intrathecally or epidurally in humans, magnesium might have
beneficial effect in perioperative pain management, but more studies are
needed for this specific route of administration [3, 2, 55,63]. Hemodynamic
side effects might be of concern.
NitrousOxide
Nitrous oxide (N2O) has been used in anesthesia for more than 50 years.
It has sedative, analgesic, and anxiolytic properties. It is an NMDA receptor antagonist [55, 56]. Animal studies reported promising anti-hyperalgesic
effect and an improvement of opioid tolerance in animals receiving N2O only
intraoperatively [57]. In humans, even if N2O has been used in anesthesia for
more than 50 years, no study has yet been designed to look at the impact
of its intraoperative administration on postoperative pain, hyperalgesia, and
opioid consumption. Future studies will have to address this question in clinical
practice.
N-Methyl-D-aspartate Antagonists
CHAPTER 7
this route, dosing starts with 0.5 mg/kg orally with an increase of 0.5 mg/kg
every 4days to a maximum of 000 mg perday.
In cancer pain, two articles concluded that there is not enough evidence
to support the use of oral ketamine [60]. Ketamine is then used in selected
patients, demonstrating either high opioid tolerance, resistance to opioids
usage, or presenting intolerable opioid-related side effects [61].
Hence, despite the fact that many clinicians reported on the use of ketamine as an adjuvant medication in the treatment of chronic pain, reports
of this practice are anecdotal and no clinical recommendations can be made.
Prospective double-blind studies on ketamine advantages in patients with
chronic pain conditions must be done on large populations in order to provide sufficient evidence on safety and efficacy, which will help to build robust
recommendation to support ketamine use in chronic pain patients [58, 62,
63]. The same conclusion applies to the other NMDA modulators/antagonists mentioned in the previous section.
References
1. Albrecht E, Kirkham KR, Liu SS, Brull R. Peri-operative intravenous administration of magnesium sulphate and postoperative pain: a meta-analysis.
Anaesthesia 203; 68:7990.
2. Angst MS, Clark JD. Opioid-induced hyperalgesia: a qualitative systematic
review. Anesthesiology 2006; 04:570587.
3. Arcioni R, Palmisani S, Tigano S, et al. Combined intrathecal and epidural magnesium sulfate supplementation of spinal anesthesia to reduce post-operative
analgesic requirements: a prospective, randomized, double-blind, controlled trial
in patients undergoing major orthopedic surgery. Acta Anaesthesiol Scand 2007;
5:482489.
4. Azari P, Lindsay DR, Briones D, et al. Efficacy and safety of ketamine in patients
with complex regional pain syndrome: a systematic review. CNS Drugs 202;
26:25228.
65
Conclusion
N-Methyl-D-aspartate Antagonists
CHAPTER 7
66
N-Methyl-D-aspartate Antagonists
CHAPTER 7
67
25. Guirimand F, Dupont X, Brasseur L, et al. The effects of ketamine on the temporal summation (wind-up) of the R(III) nociceptive flexion reflex and pain in
humans. Anesth Analg 2000; 90:40844.
26. Himmelseher S, Durieux ME. Ketamine for perioperative pain management.
Anesthesiology 2005; 02:2220.
27. Hood DD, Curry R, Eisenach JC. Intravenous remifentanil produces withdrawal hyperalgesia in volunteers with capsaicin-induced hyperalgesia. Anesth
Analg 2003; 97:8085.
28. Jevtovic-Todorovic V, Todorovic SM, Mennerick S, et al. Nitrous oxide (laughing gas) is an NMDA antagonist, neuroprotectant and neurotoxin. Nat Med
998; 4:460463.
29. Joly V, Richebe P, Guignard B, et al. Remifentanil-induced postoperative hyperalgesia
and its prevention with small-dose ketamine. Anesthesiology 2005; 03:4755.
30. Kehlet H, Jensen TS, Woolf CJ. Persistent postsurgical pain: risk factors and
prevention. Lancet 2006; 367:68625.
31. Koppert W, Dern SK, Sittl R, et al. A new model of electrically evoked pain
and hyperalgesia in human skin: the effects of intravenous alfentanil, S(+)ketamine, and lidocaine. Anesthesiology 200; 95:395402.
32. Laskowski K, Stirling A, McKay WP, Lim HJ. A systematic review of intravenous ketamine for postoperative analgesia. Can J Anaesth 20; 58:9923.
33. Lavandhomme P. Perioperative pain. Curr Opin Anaesthesiol 2006; 9:55656.
34. Lavandhomme P, De Kock M, Waterloos H. Intraoperative epidural analgesia
combined with ketamine provides effective preventive analgesia in patients
undergoing major digestive surgery. Anesthesiology 2005; 03:83820.
35. Lin SL, Tsai RY, Shen CH, et al. Co-administration of ultra-low dose
naloxone attenuates morphine tolerance in rats via attenuation of NMDA
receptor neurotransmission and suppression of neuroinflammation in the spinal cords. Pharmacol Biochem Behav 200; 96:236245.
36. Loftus RW, Yeager MP, Clark JA, et al. Intraoperative ketamine reduces perioperative opiate consumption in opiate-dependent patients with chronic back
pain undergoing back surgery. Anesthesiology 200; 3:639646.
37. Lysakowski C, Dumont L, Czarnetzki C, Tramr MR. Magnesium as an adjuvant to postoperative analgesia: a systematic review of randomized trials.
Anesth Analg 2007; 04:532539, table of contents.
38. Martinez, V., D. Fletcher, et al. 2007; The evolution of primary hyperalgesia in
orthopedic surgery: quantitative sensory testing and clinical evaluation before
and after total knee arthroplasty. Anesth Analg 05:8582.
39. McCartney CJ, Sinha A, Katz J. A qualitative systematic review of the role
of N-methyl-d-aspartate receptor antagonists in preventive analgesia. Anesth
Analg 2004; 98:385400, table of contents.
40. Meleine MC, Rivat C, Laboureyras E, et al. Sciatic nerve block fails in preventing
the development of late stress-induced hyperalgesia when high-dose fentanyl is
administered perioperatively in rats. Reg Anesth Pain Med 202; 37:448454.
41. Mercieri M, De Blasi RA, Palmisani S, et al. Changes in cerebrospinal fluid magnesium levels in patients undergoing spinal anaesthesia for hip arthroplasty:
does intravenous infusion of magnesium sulphate make any difference? A prospective, randomized, controlled study. Br J Anaesth 202; 09:20825.
N-Methyl-D-aspartate Antagonists
CHAPTER 7
68
43. Mion G, Tourtier JP, Rousseau JM. Ketamine in PCA: what is the effective
dose? Eur J Anaesthesiol 2008; 25:04004.
44. Noppers I, Niesters M, Aarts L, et al. Ketamine for the treatment of chronic
non-cancer pain. Expert Opin Pharmacother 200; :2472429.
45. Owen H, Reekie RM, Clements JA, et al. Analgesia from morphine and ketamine. A comparison of infusions of morphine and ketamine for postoperative analgesia. Anaesthesia 987; 42:05056.
46. Ozyalcin NS, Yucel A, Camlica H, et al. Effect of pre-emptive ketamine on
sensory changes and postoperative pain after thoracotomy: comparison of
epidural and intramuscular routes. Br J Anaesth 2004; 93:35636.
47. Quibell R, Prommer EE, Mihalyo M, et al. Ketamine*. J Pain Symptom Manage
20; 4:640649.
48. Quinlan J. The use of a subanesthetic infusion of intravenous ketamine to
allow withdrawal of medically prescribed opioids in people with chronic pain,
opioid tolerance and hyperalgesia: outcome at 6 months. Pain Med 202;
3:524525.
49. Ranft A, Kurz J, Becker K, et al. Nitrous oxide (N2O) pre- and postsynaptically
attenuates NMDA receptor-mediated neurotransmission in the amygdala.
Neuropharmacology 2007; 52:76723.
50. Richebe P, Rivat C, Creton C, et al. Nitrous oxide revisited: evidence for
potent antihyperalgesic properties. Anesthesiology 2005; 03:845854.
51. Schmid RL, Sandler AN, Katz J. Use and efficacy of low-dose ketamine in the
management of acute postoperative pain: a review of current techniques and
outcomes. Pain 999; 82:25.
52. Simonnet G, Rivat C. Opioid-induced hyperalgesia: abnormal or normal pain?
Neuroreport 2003; 4:7.
53. Steinlechner B, Dworschak M, Birkenberg B, et al. Magnesium moderately
decreases remifentanil dosage required for pain management after cardiac surgery. Br J Anaesth 2006; 96:444449.
54. Stubhaug A, Breivik H, Eide PK, et al. Mapping of punctuate hyperalgesia
around a surgical incision demonstrates that ketamine is a powerful suppressor of central sensitization to pain following surgery. Acta Anaesthesiol Scand
997; 4:2432.
55. Sun J, Wu X, Xu X, et al. A comparison of epidural magnesium and/or morphine with bupivacaine for postoperative analgesia after cesarean section. Int J
Obstet Anesth 202; 2:3036.
56. Suzuki M, Haraguti S, Sugimoto K, et al. Low-dose intravenous ketamine
potentiates epidural analgesia after thoracotomy. Anesthesiology 2006;
05:9.
57. Suzuki M, Kinoshita T, Kikutani T, et al. Determining the plasma concentration
of ketamine that enhances epidural bupivacaine-and-morphine-induced analgesia. Anesth Analg 2005; 0:777784.
58. Tauzin-Fin P, Sesay M, Delort-Laval S, et al. Intravenous magnesium sulphate
decreases postoperative tramadol requirement after radical prostatectomy.
Eur J Anaesth 2006; 23:055059.
59. Tramer MR, Glynn CJ. An evaluation of a single dose of magnesium to supplement analgesia after ambulatory surgery: randomized controlled trial. Anesth
Analg 2007; 04:374379, table of contents.
N-Methyl-D-aspartate Antagonists
CHAPTER 7
69
60. van Gulik L, Ahlers SJ, van de Garde EM, et al. Remifentanil during cardiac
surgery is associated with chronic thoracic pain yr after sternotomy. 202;
Br J Anaesth 09:66622.
61. Webb AR, Skinner BS, Leong S, et al. The addition of a small-dose ketamine
infusion to tramadol for postoperative analgesia: a double-blinded, placebocontrolled, randomized trial after abdominal surgery. Anesth Analg 2007;
04:9297.
62. Wilder-Smith CH, Knopfli R, Wilder-Smith OH. Perioperative magnesium infusion and postoperative pain. Acta Anaesthesiol Scand 997; 4:023027.
63. Yousef AA, Amr YM. The effect of adding magnesium sulphate to epidural
bupivacaine and fentanyl in elective caesarean section using combined spinal-epidural anaesthesia: a prospective double blind randomised study. Int J
Obstet Anesth 200; 9:40404.
Chapter8
Topical analgesics represent a class of drugs that are applied to the skin and
influence pain by local actions on sensory nerve endings and/or cellular targets
adjacent to, and interacting with, such sensory nerve endings. They encompass
such formulations as creams, lotions, gels, and sprays, as well as patches or plasters where the drug is embedded in a physical matrix. Some analgesics applied
as a patch have systemic actions that influence pain signaling (eg, fentanyl), and
are not regarded as topical analgesics. There are several advantages to the use
of topical analgesics including low systemic drug levels, fewer systemic adverse
effects (AEs), fewer drug interactions, and avoidance of factors that limit oral
bioavailability (eg, first-pass metabolism). Limitations to this approach include
access to site of action (the drug needs physicochemical properties that allow
for dermal and tissue penetration), alteration of absorption by disease states
of the skin, and local AEs in response to the drug (eg, redness, itching). Topical
analgesics can be used either as single therapies or as adjuvants in combination with oral analgesics. In the latter instance, this would potentially allow
for recruitment of multiple actions for suppressing pain without increasing
the burden of systemic AEs. Topical analgesics may be of particular benefit in
the elderly, where there are likely other medical conditions being treated with
drugs (ie, polypharmacy is common), and avoidance of central nervous system
effects (eg, sedation, confusion) is desirable.
Over the past decades, several topical analgesic formulations have been
approved for use, and these include topical nonsteroidal anti-inflammatory
drugs (NSAIDs) for inflammatory indications, topical local anesthetics as a
plaster or patch for neuropathic pain, and, more recently, a high-concentration
capsaicin patch for neuropathic pain. There is now a considerable body of
evidence that indicates topical agents are indeed efficacious in these pain
conditions when compared with placebo. More importantly, some studies
also provide comparative data between topical and oral analgesics, as well as
information on combinations of oral and topical analgesics. Taken together,
this body of information provides validation for the approach of applying
drugs locally to a site of action for pain relief in several pain conditions. The
past decade has also seen identification of molecular mechanisms involved
in peripheral pain signaling in neurons, as well as an increased understanding
of the complexity of peripheral pain signaling mechanisms with interactions
71
71
Introduction
72
between neurons and adjacent structures, and there is considerable preclinical interest in the idea of developing novel topical analgesics. It is very likely
that in the future, novel topical analgesics consisting of new molecular targets,
as well as combinations of agents, will be developed, and these will provide
clinicians with a greater range of therapeutic choices for pain management.
This chapter will consider some key recent observations that validate and
sustain an interest in this approach to pain management. Reference to a much
more extensive body of literature can be found within cited reports.
vehicle
Efficacy
Outcomes
Safety
Outcomes
+OA pain
+AUSCAN
Global
Local AEs
2.5% DSG vs .%
Veh
GI AEs
+WOMAC pain
+ WOMAC
function
+Global
8 weeks (N=385)
Barthel etal [3]
RCT knee OA
DSG 4daily;
vehicle
2 weeks (N=492)
Study
Characteristics
Diclofenac Sodium Gel %
Altman etal [2] RCT hand OA
DSG 4daily;
Local AEs
26.6% tDiclo vs
7.6% P
vs 6.8% DMSO vs
7.3% oDiclo vs
30.9%
tDiclo/oDiclo
GI AEs
6.5% tDiclo vs
9.6% P
vs .2% DMSO
vs 23.8% oDiclo vs
25.7%
tDiclo/oDiclo
compared with the oral, diclofenac (24.% vs .9%) and fewer gastrointestinal
AEs (25.4% vs 39.0%) but comparable cardiovascular AEs (.5% vs 3.5%) [5].
Acomparison of DSG effects in older (65years) versus younger patients
(<65years) in a pooled analysis of three 2-week trials reported similar efficacy in both groups (improvements of 39%46% compared with 28%35%
with placebo in younger patients vs 45%50% compared with 35%39% with
placebo in older patients) [6]. Pooled safety analysis also indicated a similar
profile in the two groups [6]. Meta-analysis of a larger and more heterogenous data set of topical NSAID drugs in older adults with OA reported up
to 39.5% application-site AEs and 7.5% systemic AEs; conclusions of this
73
Trial
Chapter8
74
Capsaicin is derived from hot chili peppers and has a long history of use in
medical practice. Capsaicin interacts with transient receptor potential vanilloid (TRPV) receptors located on A- and C-fibers, and it leads to cation entry into sensory afferents; chronic exposure to capsaicin desensitizes
the channels, leads to loss of sensory integration, and results in analgesia.
Topical low concentration capsaicin creams and patches (0.025%0.%, for
daily use) have been available since the early 980s and have been used to
treat inflammatory (OA, rheumatoid arthritis) and neuropathic (PHN, DPN)
pain conditions. The most recent meta-evaluation of efficacy of capsaicin
0.075% for neuropathic pain indicates efficacy is modest (number-needed-totreat values of 6.6) and side effects (burning and stinging) are common
(number-needed-to-harm values of 2.5) [8]. It was concluded that capsaicin
cream, either alone or in combination with other agents, may be useful in
those who do not respond to, or cannot tolerate, other treatments[8].
A high concentration (8%) capsaicin patch (Quetenza) was recently
approved in 2009 in the European Union and the United States [9]. The
patch is 280cm2, contains 79 mg of capsaicin (8% w/w), and is cut to match
the size and shape of the painful area. At this concentration, the action of
capsaicin is attributed to defunctionalization of nociceptors, which reflects
loss of membrane potential, altered transport of neurotrophic factors, and
reversible retraction of epidermal and dermal nerve fibers [9]. The 8% patch
is usually compared with a 0.04% patch as the control condition, and the low
concentration is sufficient to produce local reactions and blinding of the study
treatment; whether the 0.04% patch also produces some analgesia cannot be
determined from these studies. The 8% patch is generally applied for 60 minutes after application of topical local anesthetics (4% lidocaine or 2.5% prilocaine/2.5% lidocaine) to mitigate local pain reactions [20]. Application site
pain can be further managed with oral analgesics and/or cooling (ice). Phase
3 studies (double-blind, multicentre trials) demonstrate a significant reduction
in pain over 2 weeks in PHN and human immunodeficiency virus-associated
75
76
Chapter8
References
77
78
7. Vorobeychik Y, Gordin V, Mao J, Chen L. Combination therapy for neuropathic pain. Areview of current evidence. CNS Drugs 20; 25:023034.
8. Derry S, Lloyd R, Moore RA, etal. Topical capsaicin for chronic neuropathic
pain in adults. Cochrane Database Syst Rev 2009 Oct 7;(4):CD007393.
9. Anand P, Bley K. Topical capsaicin for pain management:therapeutic potential
and mechanisms of action of the new high-concentration capsaicin 8% patch.
Br J Anesth 20; 07:490502.
20. Webster LR, Nunez M, Trak MD, etal. Tolerability of NGX-400, a capsaicin 8% dermal patch, following pretreatment with lidocaine 2.5%/prilocaine
2.5% cream in patients with post-herpetic neuralgia. BMC Anesthesiol 20;
doi:0.86/47-2253--25.
2. Webster LR, Malan TP, Tuchman MM, et al. A multi-centre, randomized,
double-blind, controlled dose finding study of NGX-400, a high-concentration
capsaicin patch, for the treatment of postherpetic neuralgia. J Pain 200;
:972982.
22. Webster LR, Peppin JF, Murphy FT, etal. Efficacy, safety and tolerability of
NGX-400, capsaicin 8% patch, in an open-label study of patients with peripheral neuropathic pain. Diabetes Res Clin Pract 20; 93:8797.
23. McCormack PL. Capsaicin dermal patch. In non-diabetic peripheral neuropathic pain. Drugs 200; 70:83842.
24. Irving GA, Backonja M, Rauckj R, etal. NGX-400, a capsaicin 8% dermal
patch, administered alone or in combination with systemic neuropathic pain
medications, reduces pain in patients with postherpetic neuralgia. Clin J Pain
202; 28:007.
25. Zur E. Topical treatment of neuropathic pain using compounded medications.
Clin J Pain 203; 30:739.
26. Premkumar LS, Abooj M. TRP channels and analgesia. Life Sciences 203;
92:45424.
27. Smith HS. PainSkin deep at times? Pain Physician 2009; 2:9992.
Chapter9.
NeuropathicPain
NadineAttal
Diagnosis of neuropathicpain
Several screening tools have been developed over the last 0years for the
identification of NP (refs in [6]). One feature common to all these tools is a
reliance principally on verbal reports of pain qualities (ie, pain descriptors).
Two of the five screening toolsthe Leeds Assessment of Neuropathic
Symptoms and Signs (LANSS) and the Douleur Neuropathique en 4 questions (DN4) questionnairesare clinician-administered questionnaires
including both items related to the interview (ie, symptoms) and items
related to the sensory examination (ie, signs). The other three screening
tools are self-administered questionnaires including only items related to
the symptoms of NP:The Neuropathic Pain Questionnaire, ID Pain, and
PainDetect.
79
79
Introduction
NeuropathicPain
Chapter9.
80
Tricyclic antidepressants
Nortriptyline
Desipramine
Amitriptyline
Main
Mechanisms
of Action
Common
Major Side
Effects
Precautions
Other Benefits
Efficacy:Level
A/B Ratinga
Inhibition of
reuptake of
monoamines,
block of
sodium
channels,
anticholinergic
Somnolence,
anticholinergic
effects, weight
gain
Cardiac
disease (ECG),
glaucoma,
prostatic
adenoma,
seizure, use of
tramadol
Improvement of
depression, although
at generally higher
dosages than pain
(75 mg/h) and sleep
(amitriptyline)
Serotoninnorepinephrine
reuptake inhibitors
Duloxetine
Inhibition of
Nausea
serotonin and
norepinephrine
reuptake
Venlafaxine
Nausea,
Inhibition of
Cardiac disease,
hypertension
serotonin and
hypertension,
norepinephrine at high dosages use of tramadol
reuptake
A. Diabetic
Improvement of
neuropathy
depression and
generalized anxiety,
improvement of sleep
30 mg once
daily/60 mg
twicedaily
Increase by
0 mg to 25
mg every 3
to 7days up
to efficacy
and side
effects
May start at
30 mg once
daily and then
increase by
30mg after
week as
tolerated up to
20 mgdaily
81
Chapter9.
NeuropathicPain
82
Chapter9.
NeuropathicPain
Table9..Contiuned
Drug
Calcium channel
2 ligands
Gabapentin
Pregabalin
Topical lidocaine
Lidocaine 5% plasters
Main
Mechanisms
of Action
Common
Major Side
Effects
Precautions
Other Benefits
Efficacy:Level
A/B Ratinga
Starting Dose/
Maximum
Dose
Titration
Acts on 2
subunit of
voltage-gated
calcium
channels, which
decreases
central
sensitization
Sedation,
dizziness,
peripheral
edema,
weightgain
Reduce
dosages in renal
insufficiency
No clinically
significant drug
interactions,
improvement of
generalized anxiety
andsleep
A. Diabetic
neuropathy,
PHN, cancer
neuropathicpain
B. Spinal cord
injurypain
00300 mg
once to 3 times
daily/200 mg
3timesdaily
Increase by
00300 mg
3times daily
every
3 to 7days as
tolerated
Acts on 2
subunit of
voltage-gated
calcium
channels, which
decreases
central
sensitization
Sedation,
dizziness,
peripheral
edema,
weightgain
Reduce
dosages in renal
insufficiency
No clinically
significant drug
interactions,
improvement of
generalized anxiety
and sleep
A. Diabetic
neuropathy,
PHN, spinal
cord injury
2575 mg once
daily/300 mg
twice daily
Increase by
75mg daily
after 37days
and then by
50 mg every
37days as
tolerated
Block of
sodium
channels
Local
None
erythema, itch,
rash
No systemic side
effects, potential
effect on allodynia
A.PHN
3 patches/3
patches
None
Capsaicine patches 8%
Opioid agonists
Tramadol
Morphine Oxycodone
Methadone
Levorphanol
TRPV agonist
Pain
None
Erythema
Elevated blood
pressure due to
initial increase
in pain
No systemic side
effectspotential
effects on burning
pain, itch, and
allodynia
Mu receptor
agonist and
inhibition of
monoamine
reuptake
Nausea and
vomiting,
constipation,
dizziness,
somnolence
History of
substance
abuse, suicide
risk, use of
antidepressants
in elderly
patients
Mu receptor
agonists
(oxycodone
may also cause
-receptor
antagonism)
Nausea and
vomiting,
constipation,
dizziness,
somnolence
History of
substance abuse,
suicide risk, risk
of misuse on
long-term use
A.HIV neuropathy
and PHN
4 patches
to cover
the painful
arearepeat
every 3months
None
Rapid onset of
A. Diabetic
analgesic effect, effect
neuropathy,
on inflammatory pain
phantompain
B. Spinal cord
injury
50 mg once
or twice
daily/400mg
daily as
long-acting drug
Increase
by 5000
mg every
37days
Rapid onset of
A.Diabetic
analgesic effect, effect
neuropathy,
on inflammatory pain
PHN, phantom
pain
05 mg
morphine every
4 h or as needed
(equianalgesic
doses for other
opioids)/
up to 300 mg
morphine has
been used in
neuropathic pain
After 2
weeks
convert to
long-acting
opioids, use
short-acting
drugs as
needed and
as tolerated
Abbreviations:ECG, electrocardiogram; HIV, human immunodeficiency virus; PHN, postherpetic neuralgia; TRPV, transient receptor potential vanilloid receptor-.
a
Recommendation grading:Level A=good scientific evidence from several ClassItrials; Level B=some scientific evidence from ClassII trials (lower-class trials).
*Data modified from references [7, 9,2].
83
Chapter9.
NeuropathicPain
NeuropathicPain
Chapter9.
84
Capsaicin patches
Capsaicin is an agonist of transient receptor potential vanilloid receptor-
(TRPV) and activates TRPV ligand-gated channels on nociceptive fibers.
This activity in turn causes depolarization, the initiation of an action potential, and the transmission of pain signals to the spinal cord [25]. After several
days of application, TRPV-containing sensory axons are desensitized, a process also referred to as defunctionalization. Standard capsaicin-containing
creams (0.075%) have been found to be moderately effective for PHN, but
they require many applications per day and cause a burning sensation for
many days before the analgesic effect starts.
The efficacy of a single application of high-concentration capsaicin patch
(8%) for 30 minutes compared with a low concentration patch (0.04%) has
been demonstrated from weeks 2 to 2 in PHN or human immunodeficiency
virus (HIV) neuropathy [5, 26,27] with confirmed safety in an open-label
48-week extension [26, 28,29]. However, the optimal duration of the patches
to produce analgesic efficacy was distinct in PHN (60 minutes) and HIV neuropathy (30 minutes). The effects of this treatment on multiple symptoms
NeuropathicPain
Chapter9.
85
Opioids
The use of opioids for the treatment of chronic pain has increased dramatically over the past decade. There has been a longstanding debate about their
efficacy in chronic NP [9]. However, several randomized controlled trials
(RCTs) have now established that opioids (oxycodone, methadone, morphine) have efficacy in diabetic PPN and PHN at dosages ranging from 0 to
20 mg for oxycodone, the most studied drug in NP [79, ,2]. The dosages necessary to reach efficacy may be higher for NP than for nociceptive
pain. Furthermore, the effects obtained with NP are not necessarily associated with significant improvement in quality of life, psychological comorbidities, and sleep disorders. Another opioid, tapentadol (500 mg daily), a
-opioid agonist with norepinephrine reuptake inhibition, has been more
recently studied in peripheral NP with encouraging effects in one diabetic
NPtrial.
The most common side effects of opioids are constipation, sedation, nausea, dizziness, and vomiting, although these generally decrease after long-term
treatment, with the exception of constipation [20]. Opioids must be used
with great caution in patients with a history of drugabuse.
The problems associated with long-term opioid use are increasingly
reported in chronic noncancer pain. Long-term morphine administration may
be associated with immunologic changes and hypogonadism [0]. The risk
of misuse or addiction in chronic pain, although low (2.6%) in recent systematic studies [2], may represent a concern in long-term use. Prescription
opioid dependence is associated with structural and functional changes in
brain regions implicated in the regulation of affect, reward, and motivational
functions [22]. Opioid-induced hyperalgesia, defined as an increase in pain
sensitivity with the use of opioids, has been demonstrated in animal models,
and there is concern that it might occur in humans [23]. For these reasons,
opioids are considered to be second-line treatment for noncancer NP, including NP, in all current recommendations [7, 0,24].
NeuropathicPain
Chapter9.
86
Figure9.. Therapeutic algorithm proposed for peripheral neuropathic pain (NP) in clinical practice. This algorithm is based on current evidence-based recommendations and systematic reviews in peripheral NP [7, 9, ,30]. Serotonin-norepinephrine reuptake inhibitor (SNRI) antidepressants are generally recommended as first
choice, but duloxetine has higher evidence for peripheral NP. The choice between first-line drugs depends on the clinical profile (for example, tricyclic antidepressants
should be avoided in the elderly), contraindications, and comorbid conditions (for example, patients with anxiety, sleep disorders, or depression may benefit more from
pregabalin/gabapentin or SNRI antidepressants). Capsaicin high-concentration patches have not been considered yet in this therapeutic algorithm.
NeuropathicPain
Chapter9.
88
Pregabalin is now the drug of choice for SCI pain. One comparative trial
found efficacy of high-dose levorphanol for central pain [7]. AClassItrial
showed no superiority of duloxetine over placebo on the primary outcome of central pain due to stroke or SCI, but several secondary outcomes, including allodynia to brush and cold, favored duloxetine [34].
Thus, central NP seems to generally respond to the same drug treatments
as peripheralNP.
Several large-scale trials of posttraumatic neuropathy have been reported.
One trial found that gabapentin (up to 2400 mg/day) had no effect on pain
intensity but improved pain relief, sleep, and quality of life [35]. Another trial
found that pregabalin was moderately effective (difference 0.62 versus placebo) on the primary outcome [36]. Lower-class studies found moderate
effects of amitriptyline and low-dose venlafaxine on postmastectomy pain
and discrepant results with topical capsaicin[7].
Studies of gabapentin have found positive results in GuillainBarr syndrome and cancer NP and discrepant results in phantom limb pain. Opioids
and tramadol have been found to be efficacious for phantom limb pain, and
amitriptyline has been found to be efficacious for cancer NP [7, 0,].
Human immunodeficiency virus neuropathy and chronic radiculopathy
have generally been found to be poorly responsive to drugs that are useful
for other NP conditions. In HIV neuropathy, negative results were obtained
with amitriptyline, topical lidocaine, gabapentin [7, 9,], and pregabalin [37],
whereas lamotrigine, smoked cannabis, and more recently high-concentration
capsaicin patches (see below) were found to be moderately useful.
A recent large-scale study using an enrichment phase demonstrated
no benefit of pregabalin for lumbosacral radiculopathy [7]. A crossover
placebo-controlled study of nortriptyline, morphine, and their combination
in lumbosacral radiculopathy was negative for the primary outcome and
found only slight effects for the combination of worst pain and pain relief
[38]. However, given the lack of specific assessment of pain quality in most
trials, the possibility that these drugs might be effective in a subset of patients
exhibiting particular clinical phenotypes or improve only some dimensions
of NP cannot be excluded. New studies are warranted for these indications,
particularly among patients with failed back syndrome, because a large subset
of these patients have NP, and radicular pain probably represents one of the
most common NP conditions in the general population[2].
Combination and head-to-head studies
Several head-to-head comparative studies have been performed in NP,
but most studies are single-center trials with small sample size. Most initial
studies aimed to compare drugs from the same class, particularly TCAs.
These trials found similar efficacy of different TCAs [7, 0,]. In one study,
venlafaxine 225 mg/day was equivalent to imipramine 50 mg/day with
respect to overall pain intensity and tolerability, but it was less effective on
the proportion of responders, pain relief, and quality of life [7]. Other trials reported similar efficacy of gabapentin and nortriptyline in diabetic NP
and PHN [39], pregabalin and amitriptyline [40] and lamotrigine and amitriptyline in diabetic NP [4]. These results may be related to small sample
NeuropathicPain
Chapter9.
89
size and do not exclude the possibility that these drugs have distinct effects
depending on patients clinical profiles, which were generally not detailed
at baseline.
Several placebo-controlled trials confirmed the benefit of gabapentin
combined with nortriptyline or morphine compared with gabapentin monotherapy in a mixed group of patients with diabetic PPN and PHN [39, 42,43].
The combination drug arms demonstrated better efficacy with lower dosages
compared with monotherapy without an increase in side effects. Similarly,
in diabetic NP, gabapentin in combination with oxycodone was superior to
gabapentin alone [43]. In a large-scale study, patients unresponsive to moderate dosages of pregabalin (300 mg daily) or duloxetine (60 mg daily) were
subsequently randomized to receive either the combination of both drugs
at similar dosages or increased dosages of the same drugs in monotherapy
(ie, 600 mg of pregabalin or 20 mg of duloxetine) [44]. The study showed
similar efficacy of combination therapy and monotherapy at high dosages
on primary and secondary outcomes, including quality of life and sleep and
no significant difference in side effects. These trials suggest that combination
therapy with these agents may be useful, particularly when monotherapy is
incompletely effective.
NeuropathicPain
Chapter9.
NP associated with allodynia [7, 0,], but several unpublished trials are
negative. Adverse events include dizziness, dry mouth, sedation, fatigue,
gastrointestinal effects, and oral discomfort. Although no impairment of
cognition or psychoactive effects were noted in these trials, cannabis may
exacerbate psychiatric conditions, so cannabinoids are not recommended
for patients with psychiatric disorders. There is controversy with regard to
tolerance and dependence after long-term treatment [49]. Oromucosal
cannabinoids are currently not available for the treatment of NP in the
United States, but they are available in Canada.
90
NeuropathicPain
Consensus recommendations for the pharmacologic treatment of NP generally suggest antiepileptics (notably pregabalin) and TCAs (notably amitriptyline) as first-line therapy; SNRIs (duloxetine) and lidocaine 5% plasters are
also proposed as first-line agents in certain NP conditions. Clinical advances
in the management of NP include the implementation of comparative studies
and combination therapy trials, the study of rarer and often neglected NP
conditions, and the identification of responder profiles based on a detailed
characterization of symptoms and signs using sensory examination and specific pain questionnaires. New drug treatments will undoubtedly contribute to
the improved managementofNP.
Chapter9.
Conclusions
91
References
NeuropathicPain
Chapter9.
92
3. Gahimer J, Wernicke J, Yalcin I, etal. A retrospective pooled analysis of duloxetine safety in 23,983 subjects. Curr Med Res Opin 2007; 23:7584.
4. Freeman R, Durso-Decruz E, Emir B. Efficacy, safety and tolerability of pregabalin treatment for painful diabetic peripheral neuropathy:findings from seven
randomized controlled trials accross a range of doses. Diabetes Care 2008;
3:448454.
5. Wiffen PJ, McQuay HJ, Edwards JE, etal. Gabapentin for acute and chronic
pain. Cochrane Database Syst Rev 2009. Available at http://onlinelibrary.
wiley.com/doi/0.002/465858.CD005452.pub2/pdf. Accessed 27
November,204.
6. Irving G, Jensen M, Cramer M, etal. Efficacy and tolerability of gastric-retentive
gabapentin for the treatment of postherpetic neuralgia: results of a
double-blind, randomized, placebo-controlled clinical trial. Clin J Pain 2009;
25:8592.
7. Khaliq W, Alam S, Puri N. Topical lidocaine for the treatment of postherpetic
neuralgia. Cochrane Database Syst Rev 2007; 8:CD004846.
8. Baron R, Mayoral V, Leijon G, et al. 5% lidocaine medicated plaster versus pregabalin in post-herpetic neuralgia and diabetic polyneuropathy: an
open-label, non-inferiority two-stage RCT study. Curr Med Res Opin 2009;
25:663676.
9. Eisenberg E, McNicol ED, Carr DB. Efficacy and safety of opioid agonists in the
treatment of neuropathic pain of nonmalignant origin:systematic review and
meta-analysis of randomized controlled trials. JAMA 2005; 293:30433052.
20. Moore RA, McQuay HJ. Prevalence of opioid adverse events in chronic
non-malignant pain:systematic review of randomised trials of oral opioids.
Arthritis Res Ther 2005; 7:R046R05.
2. Portenoy RK, Farrar JT, Backonja MM, etal. Long-term use of controlled-release
oxycodone for noncancer pain:results of a 3-year registry study. Clin J Pain
2007; 23:287299.
22. Upadhyay J, Maleki N, Potter J, etal. Alterations in brain structure and functional connectivity in prescription opioid-dependent patients. Brain 200;
33(pt 7):209824.
23. Crofford LJ. Adverse effects of chronic opioid therapy for chronic musculoskeletal pain. Nat Rev Rheumatol 200; 6:997.
24. Bril V, England J, Franklin GM, etal. Evidence-based guideline:treatment of
painful diabetic neuropathy:report of the American Academy of Neurology,
the American Association of Neuromuscular and Electrodiagnostic Medicine,
and the American Academy of Physical Medicine and Rehabilitation.
Neurology 20; 76:758765.
25. Wong GY, Gavva NR. Therapeutic potential of vanilloid receptor TRPV agonists and antagonists as analgesics:Recent advances and setbacks. Brain Res
Rev 2009; 60:267277.
26. Backonja MM, Malan TP, Vanhove GF, etal. NGX-400, a high-concentration
capsaicin patch, for the treatment of postherpetic neuralgia:a randomized,
double-blind, controlled study with an open-label extension. Pain Med 200;
:600608.
27. Simpson DM, Brown S, Tobias J. Controlled trial of high-concentration capsaicin patch for treatment of painful HIV neuropathy. Neurology 2008;
70:2305233.
28. Kennedy WR, Vanhove GF, Lu SP, etal. A randomized, controlled, open-label
study of the long-term effects of NGX-400, a high-concentration capsaicin
45. Ranoux D, Attal N, Morain F, etal. Botulinum toxin type a Ainduces direct
analgesic effects in chronic neuropathic pain:a double blind placebo controlled
study. Ann Neurol 2008; 64:274283.
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93
patch, on epidermal nerve fiber density and sensory function in healthy volunteers. J Pain 200; :579587.
29. Simpson DM, Gazda S, Brown S, etal. Long-term safety of NGX-400, a
high-concentration capsaicin patch, in patients with peripheral neuropathic
pain. J Pain Symptom Manage 200; 39:053064.
30. Attal N, Cruccu G, Haanp M, etal. EFNS guidelines on pharmacological
treatment of neuropathic pain. Eur J Neurol 2006; 3:5369.
3. Tan T, Barry P, Reken S. Pharmacological management of neuropathic pain in
non-specialist settings:summary of NICE guidance. Br Med J 200; 340:c079.
32. Vranken JH, Dijkgraaf MG, Kruis MR, etal. Pregabalin in patients with central
neuropathic pain:a randomized, double-blind, placebo-controlled trial of a
flexible-dose regimen. Pain 2008; 36:5057.
33. Kim JS, Bashford G, Murphy TK, etal. Safety and efficacy of pregabalin in
patients with central post-stroke pain. Pain 20; 52:08023.
34. Vranken J, Hollmann MW, van der Vegt MH, etal. Duloxetine in patients with
central neuropathic pain:a a randomized, double-blind, placebo-controlled
trial of a flexible-dose regimen. Pain 200; 52:267273.
35. Gordh TE, Stubhaug A, Jensen TS, etal. Gabapentin in traumatic nerve injury
pain:a randomized, double-blind, placebo-controlled, cross-over, multi-center
study. Pain 2008; 38:255266.
36. van Seventer R, Bach FW, Toth CC, etal. Pregabalin in the treatment of
post-traumatic peripheral neuropathic pain:a randomized double-blind trial.
Eur J Neurol 200; 7:082089.
37. Simpson DM, Schifitto G, Clifford DB. Pregabalin for painful HIV neuropathy:a randomized, double-blind, placebo-controlled trial. Neurology 200;
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38. Khoromi S, Cui L, Nackers L, etal. Morphine, nortriptyline and their combination vs. placebo in patients with chronic lumbar root pain. Pain 2007;
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39. Gilron I, Baley JM, Tu D, etal. Nortritpyline and gabapentin, alone and in combination for neuropathic pain:a double-blind, randomised controlled crossover trial. Lancet 2009; 374:25226.
40. Bansal D, Bhansali A, Hota D, etal. Amitriptyline versus vs. pregabalin in painful diabetic neuropathy:a randomized double blind clinical trial. Diabet Med
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4. Jose VM, Bhansali A, Hota D, etal. Randomized double-blind study comparing the efficacy and safety of lamotrigine and amitriptyline in painful diabetic
neuropathy. Diabet Med 2007; 24:377383.
42. Gilron I, Bailey JM, Tu D, etal. Morphine, gabapentin, or their combination for
neuropathic pain. N Engl J Med 2005; 352:324334.
43. Hanna M, OBrien C, Wilson MC. Prolonged-release oxycodone enhances the
effects of existing gabapentin therapy in painful diabetic neuropathy patients.
Eur J Pain 2008; 2:80483.
44. Tesfaye S, Wilhelm S, Lledo A, etal. Duloxetine and pregabalin:high-dose
monotherapy or their combination? The COMBO-DN studya multinational, randomized, double-blind, parallel-group study in patients with diabetic
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NeuropathicPain
Chapter9.
94
Chapter9.2
Cancer-relatedPain
Paul N.Luong and Russell K.Portenoy
95
95
Introduction
Cancer-relatedPain
Chapter9.2
Class
Subclass
Drugs
Antidepressants
Tricyclics
amitriptyline,
desipramine,
nortriptyline
duloxetine,
minalcipran,
venlafaxine,
desvenlafaxine
paroxetine,
citalopram
buproprion
dexamethasone,
prednisone,
methylprednisone
tizanidine, clonidine
dronabinol, nabilone,
nabiximols
local anesthetics,
capsaicin, tricyclic
antidepressants,
NSAIDs, others
see above
SNRIs
SSRIs
96
Corticosteroids
Other
2-Adrenergic agonists
Cannabinoids
Used for
neuropathic
pain
Topical analgesics
All multipurpose
analgesics
Anticonvulsants
See above
Sodium channel
blockers
Sodium channel
modulator
Sodium channel
blocker
N-Methyl-D -aspartate
receptor antagonists
gabapentin,
pregabalin,
divalproex,
phenytoin,
carbamazepine,
oxcarbazepine,
topiramate,
lamotrigine,
lacosamide
mexiletine,
IVlidocaine
ketamine,
memantine,
dextromethorphan,
amantadine
(continued)
Class
Subclass
Drugs
GABA agonists
Osteoclast inhibitors
GABAa agonists
GABAb agonists
Bisphosphonates
Radiopharmaceuticals
clonazepam
baclofen
pamidronate,
zolendronate,
ibandronate
calcitonin
strontium-89,
samarium-53
Plus:NSAIDs,
corticosteroids
Anticholinergic drugs
Somatostatin analogue
Plus:Corticosteroids
Cancer-relatedPain
Category
Based on
Conventional
Use
Chapter9.2
Table 9.2.Continued
scopolamine,
atropine,
glycopyrrolate
octreotide
97
Multipurpose analgesics
The so-called multipurpose analgesics include antidepressants, corticosteroids, 2-adrenergic agonists, cannabinoids, and topical therapies. As
noted, the population of cancer survivors is best considered to be comparable with other populations with chronic pain. For these patients, some
of the multipurpose adjuvant analgesics, such as the antidepressants and
topical therapies, are considered first-line approaches. For those with
active cancer, all of these drugs are typically considered as add-on therapies for any type of pain that is poorly opioid-responsive. In practice, the
usual indication is neuropathic pain that has been poorly responsive to an
opioid.
Analgesic antidepressants
Among many available antidepressants, analgesic efficacy is best established
for some of the tricyclic compounds and the serotonin-norepinephrine
reuptake inhibitors (SNRIs) [Table 9.2.]. Evidence of analgesic efficacy in
cancer-related pain is very limited, however. The tricyclic antidepressants
have been suggested to have some analgesic efficacy in a few partially controlled trials [7,8] and one randomized controlled trial of amitriptyline [9].
Although the side effects associated with the tricyclic drugs may be of concern in medically ill patients, some patients may have symptoms other than
pain that may benefit from specific side effects, such as sedation. The secondary amine tricyclic drugs, such as desipramine, have fewer side effects than
Cancer-relatedPain
Chapter9.2
98
the tertiary amine drugs such as amitriptyline, and former agents are usually
preferred when pain is the target symptom.
Serotonin-norepinephrine reuptake inhibitors are usually better tolerated
than tricyclics and have been shown to be analgesic in a few cancer-related
conditions. Venlafaxine can decrease acute neurosensory symptoms and
chronic oxaliplatin neurotoxicity when administered during 2-week course
of chemotherapy [0]. It can also prevent chronic postmastectomy pain
when initiated the night before surgery and administered for two weeks [].
Duloxetine was effective in relieving pain from chronic oxaliplatin-induced
peripheral neuropathy in 63% of patients with colon cancer who could tolerate it [2], as well as in patients who did not tolerate pregabalin [3]. Relief
of chemotherapy-induced peripheral neuropathy was also shown in a recent
randomized controlled trial[4].
There is no evidence of analgesic efficacy of all other antidepressants in
cancer-related pain. Bupropion, which is associated with less fatigue and somnolence than either the tricyclic drugs or the SNRIs, might nevertheless be a
good option for cancer patients who also are experiencing distressing sedation or fatigue. Mirtazapine, which has no evidence of pain relief, has been
shown to improve sleep, anxiety, and depression in cancer patients, and it can
be used to address these symptoms[5].
When used to treat cancer-related pain, antidepressants should be prescribed using the same doses and protocols applied in the treatment of
chronic noncancer pain syndromes. These are described in Chapter3.
Corticosteroids
Corticosteroids have been widely used to treat cancer-related symptoms
such as pain, nausea, fatigue, poor appetite, malaise, and poor overall quality
of life [5]. Although evidence from clinical trials is limited, there is extensive
clinical experience that suggests benefit for varied pain syndromes related to
active cancer, including neuropathic pain resulting from nerve compression,
bone pain, pain associated with capsular expansion or duct obstruction, pain
from bowel obstruction, pain caused by lymphedema, and headache caused
by increased intracranial pressure [6]. The mechanism of action is unknown,
but it may relate to the reduction of peritumoral edema, anti-inflammatory
effects, and direct effects on nociceptive neural systems.
Although many clinicians favor dexamethasone, presumably because of its
relatively low mineralocorticoid effects, there are no comparative trials of the
various drugs in this class. Prednisone and methylprednisolone are acceptable
alternatives.
In the setting of advanced cancer, a corticosteroid typically is added to
opioid therapy at a low dose, with no intent to taper or discontinue therapy.
The risks of long-term treatment, which includes myopathy, immunosuppression, psychotomimetic effects, and hypoadrenalism, are less relevant when
life expectancy is short. When life expectancy is indeterminate or relatively
long, these potential adverse effects must be considered; open-ended treatment with a corticosteroid should not be undertaken unless safer alternatives
are lacking.
Cancer-relatedPain
Chapter9.2
There are no data that adequately inform dose selection for long-term
corticosteroid therapy in those with advanced cancer. Typically, dexamethasone 2 mg/day or prednisone 50 mg/day is administered [Table 9.2.2].
Dexamethasone can be given orally or parenterally, and the low-dose regimen may be initiated with a larger loading dose of 020mg.
Based on experience in the treatment of emergent spinal cord compression [7], a high-dose dexamethasone regimen has been used to treat very
severe and escalating pain (sometimes called pain emergencies). Adexamethasone loading dose of 5000 mg intravenously may be followed by
224 mg four times daily, which is tapered over 3 weeks, usually as some
other intervention (eg, radiotherapy or a pain intervention such as neural
blockade) is used to treat thepain.
Used for
neuropathic
pain
Used for bone
pain
Used for bowel
obstruction
Class
Drugs
Usual
Starting
Dose
Usual Effective
Dose Range
Osteoclast
inhibitors
Anticholinergic
drugs
Somatostatin
analog
pamidronate
6090 mg
qmonth
unit/kg per day
calcitonin
glycopyrrolate
0. mg qd 0.0.2 mg tid
octreotide
Varies
0.0.3 mg bid
Abbreviations:bid, twice a day; IV, intravenously; PO, orally; q, each; qd, once a day; qhs, every
night at bedtime; tid, three timesaday.
99
2-Adrenergic agonists
Clonidine and tizanidine are 2-adrenergic agonists. Clonidine has been used
in diverse types of chronic pain; intraspinal clonidine has been shown to
reduce neuropathic pain in patients with severe cancer pain partly responding
Cancer-relatedPain
Chapter9.2
100
Cancer-relatedPain
Chapter9.2
Anticonvulsant analgesics
The analgesic effects of the gabapentinoids are well established. In cancerrelated neuropathic pain, evidence is best for pregabalin. This drug relieved
neuropathic cancer pain in a randomized controlled trial, and it was better
than gabapentin or amitriptyline [9]. It also reduced the symptoms of chemotherapy-induced peripheral neuropathy [2]. Studies of gabapentin have
demonstrated its analgesic efficacy in chemotherapy-induced peripheral neuropathy and diverse types of neuropathic cancer pain [9]. Combination of
gabapentin and an opioid was shown to be more effective than the opioid
alone [22, 23].It also worked in combination with imipramine (low-dose
gabapentin 200 mg bid and imipramine 0 mg bid were more effective and
better tolerated than high-dose gabapentin 400 mg bid alone) [24]. When
combined with topical EMLA cream, gabapentin also decreased acute pain
and prevented chronic pain after mastectomy [25].
Patients may respond to either pregabalin, gabapentin, or both drugs.
Given the lack of evidence for analgesic efficacy of other anticonvulsants in
neuropathic cancer pain, trials of other drugs should be considered after a
patient demonstrates lack of benefit from both of the gabapentinoids and
one or more analgesic antidepressant drugs. In this setting of refractory neuropathic pain, other anticonvulsants (and other drug classes described below)
may be considered. These include oxcarbazepine, lamotrigine, lacosamide,
topiramate, and sodium divalproex.
101
Cancer-relatedPain
Chapter9.2
has been used, beginning as low as 0.05 mg/kg per hour; most clinicians seem
to favor a starting dose of 0.20.5 mg/kg per hour. The infusion is gradually
increased, often until benefit occurs or side effects appear. Concurrent treatment with a benzodiazepine or neuroleptic is usually done to reduce the risk
of psychotomimetic effects. Oral ketamine has also been used, and based on
clinical experience, a starting dose of 0.5 mg/kg in two or three divided doses
is used. This is titrated higher, again seeking an analgesic effect with tolerable
side effects. Abenzodiazepine or neuroleptic drug is coadministered.
Other NMDA receptor antagonists, such as memantine, amantadine, and
dextromethorphan, have also been studied in diverse types of neuropathic
pain, but results have been mixed. They are rarely considered for trials in
cancer-related neuropathic pain that has not responded to other therapies.
Other drugs that are sometimes used for noncancer pain syndromes
with a neuropathic component can be considered for treatment-refractory
cancer-related neuropathic pain. The GABAA agonist, clonazepam, and the
GABAB agonist, baclofen, are two such agents.
102
Cancer-relatedPain
Radionuclides
Bone-seeking radionuclides, such as strontium-89 and samarium-53, link a
short-lived radiation source to a bisphosphonate molecule. The drug is taken
up at the site of bone metastases and can be a useful treatment for refractory
multifocal bone pain [3]. Bone marrow suppression is a significant concern,
however, and treatment requires specialized skills and facilities.
Chapter9.2
an alternative strategy for bone pain should be considered for patients with
very poor dentition, jaw infection, or recent substantial dental procedures.
There is conflicting information about the potential for subcutaneous calcitonin to reduce metastatic bone pain [3]. Given the limited evidence, an
empirical trial of this treatment is generally considered only when other treatments are not available or are ineffective.
103
Cancer-relatedPain
Chapter9.2
Conclusions
Adjuvant analgesics are important additions to opioid therapy in pain related
to active cancer and often are first-line strategies for cancer-related pain
in the survivor community. The development of these drugs during recent
decades has been very rapid, and there now are numerous drugs in many
classes. The clinical approach to the selection and administration of one or
more of these drugs in populations with cancer remains largely empirical,
based on data obtained in other populations and experience. Studies that
compare the safety and effectiveness of these drugs in various indications are
badly needed.
104
References
. van den Beuken-van Everdingen MH, de Rijke JM, Kessels AG, etal. Prevalence
of pain in patients with caner:a systematic review of the past 40years. Ann
Oncol 2007; 8:437449.
2. Deandrea S, Montanari M, Moja L, Apolone G. Prevalence of undertreatment in cancer pain. A review of published literature. Ann Oncol 2008;
9:98599.
3. Mercadante S, Portenoy RK. Opioid poorly responsive cancer pain.
Part3:Clinical strategies to improve opioid responsiveness. J Pain Symptom
Manage 200; 2:338354.
4. Dworkin RH, OConnor AB, Backonja M, et al. Pharmacologic management of neuropathic pain: evidence-based recommendations. Pain 2007;
32:23725.
5. Lussier D, Portenoy RK. Adjuvant analgesics in pain management. In:Hanks
G, Cherny NI, Christakis N, etal, eds. Oxford Textbook of Palliative Medicine.
4th ed. Oxford, England:Oxford University Press; 200:pp. 706734.
6. Lussier D, Huskey AG, Portenoy RK. Adjuvant analgesics in cancer pain management. Oncologist 2004; 9:5759.
7. Ventafridda V, Bonezzi C, Caraceni A, etal. Antidepressants for cancer pain
and other painful syndromes with deafferentation component:comparison of
amitriptyline and trazodone. Ital J Neurol Sci 987; 8:579587.
8. Walsh TD. Controlled study of imipramine and morphine in chronic pain due
to advanced cancer. Proc Am Soc Clin Oncol 986;5:237.
9. Mishra S, Bhatnagar S, Goyal GN, etal. A comparative efficacy of amitriptyline,
gabapentin, and pregabalin in neuropathic cancer pain:a prospective randomized
double-blind placebo-controlled study. Am J Hosp Pall Care 202; 29:7782.
0. Durand JP, Deplanque G, Montheil V, etal. Efficacy of venlafaxine for the
prevention and relief of oxaliplatin-induced acute neurotoxicity:results of
26. Brose WG, Cousins MJ. Subcutaneous lidocaine for treatment of neuropathic
cancer pain. Pain 99; 45:4548.
Cancer-relatedPain
Chapter9.2
105
Cancer-relatedPain
Chapter9.2
106
Chapter9.3
107
107
Introduction
108
Neurogenic mechanisms in
rheumatic conditions
Pain due to a rheumatic process is a complex interaction of local factors at
the periphery, modulation of the pain message by plastic changes in the spinal
cord and brain stem, altered function in the brain, and finally effects mediated
via the descending inhibitory system [5]. Local tissue changes cause activation
of the primary somatosensory neuron and account for the initial nociceptive
response. In the setting of ongoing pain, this initial response is followed by
neurophysiologic and even structural changes within the nervous system.
Several lines of evidence strengthen the hypothesis of interplay of neurogenic factors in the pain experience of rheumatic conditions. In the setting of
continued pain, neuronal peripheral and central sensitization leads to an exaggeration of response to various stimuli, and is a factor in perpetuation of pain
[5]. Molecules augmenting the pain message include glutamate, substance
P, and calcitonin gene-related peptide, whereas those that mostly dampen
the pain message are the endogenous opioids, cannabinoids, serotonin, and
norepinephrine [57]. Changes in brain function and structure have been
observed in patients with painful OA, with ()reversal of activation after
administration of lidocaine into the painful joint and (2)return of thalamus to
normal size after joint replacement [8].
Adjuvant treatments
In the light of the contribution of neurogenic mechanisms in rheumatic pain,
as well as the considerable overlap with FM in many rheumatic conditions, the
effect of adjuvant treatments is of interest. Two broad categories of adjuvant
medications, namely anticonvulsants and antidepressants, have been extensively studied in FM. Anticonvulsant agents dampen neuronal hyperexcitability with effect on sensitization, whereas the antidepressant group affects
descending pain inhibitory pathways in the brain stem and spinal cord via
serotonin and norepinephrine mechanisms [2,3]. Adjuvants may also have
the added advantage of affecting some of the common accompaniments to
pain such as anxiety, depression, and sleep disturbance. Table 9.3. provides a
summary of the evidence of analgesic efficacy for various adjuvant analgesics
for the treatment of FM and rheumatic pain along with recommendeddoses.
Analgesic anticonvulsantdrugs
Anticonvulsant drugs in the class of gabapentinoids (2 ligand drugs) are classified as second-generation anticonvulsants, and they have shown clinical efficacy in the treatment of FM [4,5]. In a meta-analysis of treatment effects
of gabapentin and pregabalin in FM, there was strong evidence for reduction
Topical agents
Cannabinoids
Fibromyalgia
Gabapentin
Pregabalin
TCAs
SSRIs
SNRIs
duloxetine
milnacipran
NSAIDs
Capsaicin
Herbal
Nabilone
Sativex
+
+
+
+/
Suggested Daily
Dose
00300 mg HS
2500 mg HS
025 mg HS
Variable
+
+
No studies
No studies
No studies
+
No studies
3060 mg
00200 mg
N/A
N/A
N/A
0.5 mg
N/A
+
+
No studies
No studies
+
3060 mg
N/A
TID/QID
TID
N/A
N/A
28 puffs
Abbreviations:HS, at bedtime; N/A, data not available; NSAIDs, nonsteroidal anti-inflammatory drugs; SNRIs, serotonin
norepinephrine reuptake inhibitors; SSRIs, selective serotonin reuptake inhibitors; TCAs, tricyclic antidepressants; TID, 3 times a day;
QID, 4 times a day; +, evidence supports analgesic efficacy; , evidence suggests does not have analgesic efficacy; +/, conflicting
evidence on analgesic efficacy.
109
Chapter9.3
110
of pain, improved sleep, and improved health-related quality of life, and some
impact on fatigue and anxiety [4]. Troublesome side effects of drowsiness,
weight gain, and edema have led physicians to reduce doses in clinical practice, in contrast to the higher doses used in clinical trials [3,4].
To date, there have been no controlled studies examining the use of
gabapentinoids in human rheumatic diseases, although pain behaviors were
reduced by pregabalin administration in an OA rat model [6]. Only one small
post hoc clinical study has reported beneficial effects of pregabalin in OA
of the hip [7]. Extrapolating from experience in FM, but without study in
arthritic disease, these agents are used off-label to treat both pain and sleep
disturbance in arthritis patients. Combination drug treatment is also commonly used in clinical practice and may allow for lower doses of individual
drugs, thereby attenuating side effects. Asingle study has reported better
effect when a combination of pregabalin and celecoxib, a cyclooxygenase-2
inhibitor, was used compared with monotherapy for the treatment of back
pain[8].
Pain modulators affecting descending inhibitory pathways
Although mostly recognized for effect on descending pain inhibitory pathways
in the brain stem and spinal cord, mediated by norepinephrine and serotonin,
antidepressants may also have an impact on opioid mechanisms, ion channels,
N-methyl-D -aspartate (NMDA) channels, and even inflammation. In a mouse
model of rheumatoid arthritis (RA), both citalopram and fluoxetine inhibited
disease progression and also inhibited production of inflammatory cytokines
in human synovial membrane cultures[9].
Although clinical studies are mostly in FM, there is evidence for effect in
other rheumatic conditions in which analgesics and NSAIDs are not sufficiently effective [20]. The best studied in this group are the older tricyclic
antidepressants (TCAs). Amitriptyline and its metabolite nortriptyline have
shown efficacy in the treatment of FM but with modest effect that tends to
wear off over time [2]. However, the selective serotonin reuptake inhibitors
(SSRIs) have not shown consistent analgesic effect [22]. In a meta-analysis of
nine trials, antidepressants in the TCA and SSRI classes improved pain but not
function in patients with chronic low back pain[23].
The development of new antidepressant agents with reduced side-effect
profile holds promise for the management of rheumatic pain. Newer antidepressants that inhibit reuptake of serotonin and norepinephrine, termed
serotonin norepinephrine reuptake inhibitors, may offer improved tolerability
and have shown promise in pain management. Duloxetine and milnacipran,
agents with a balanced effect on serotonin and norepinephrine, have shown
consistent improvement in pain and function in FM, with sustained response
up to one year [2430]. Both duloxetine and milnacipran have been approved
by the FDA for treatment of FM, and duloxetine has an added indication
for the treatment of chronic pain including low back pain. However, dosing for duloxetine is lower than that for depression, with effect mostly seen
with a daily dose of 60 mg/day. Although the primary outcome for most of
these studies has focused on pain relief, improvements in global health status,
mood, and even fatigue have been reported. The ideal dosing of these agents
The cannabinoids
Contrary to popular belief, the cannabinoid effects are not only confined to
the nervous system and pain pathways, but they have an impact on inflammation and even joint damage [32]. Information regarding the use of cannabinoids for management of pain in musculoskeletal conditions is available from
preclinical science, population surveys, anecdotal reports, and the results of
only three formal clinical trials:two in FM and one in RA [3338].
Treatment of musculoskeletal pain is a common reason for use of medicinal cannabis, with 80% of users in a pain clinic in the United States reporting
myofascial pain, and up to one third of persons in two population studies
in the United Kingdom and Australia reporting use for treatment of arthritis pain [33, 34,39]. Aconcerning issue raised by both the population studies is the overlap of recreational and medicinal cannabinoid use. Healthcare
professionals need to clarify to patients that any recommendation for herbal
cannabis use can only be made specifically for the purpose of symptom management. In addition, it is necessary that persons using medicinal cannabis
must discriminate between recreational and medicinal use. The fine line that
exists between use and abuse has medicolegal implications for any healthcare
professional caring for patients who use medicinal cannabis.
The effect of nabilone, a synthetic cannabinoid, has been studied in two
small randomized controlled trials in patients with FM [37,38]. In the first
study, nabilone was associated with improved pain and function, whereas the
second study reported equivalency of nabilone and amitriptyline for effect
on sleep but without significant effect on either pain or quality of life. Both
studies reported more side effects in those using nabilone. In an uncontrolled
study, pain scores were reduced two hours after herbal cannabis use in 28 FM
patients but with no impact upon function as measured by the Short Form
36 Health Survey or the FIQ [40]. Therefore, on the strength of evidence,
cannabinoid use in FM remains of questionablevalue.
Cannabinoids have been studied in RA in a single randomized controlled
trial [36]. Fifty-eight RA patients were treated with the oromucosal spray
Sativex or placebo over a 5-week period, with significant improvement in pain
and sleep in the active group. This first study of cannabinoid treatment in
an inflammatory rheumatic disease suggests a possible therapeutic role, but
additional study is required.
In a systematic review and meta-analysis that included 4 studies with
28 patients with musculoskeletal disease, pain scores showed statistical
improvements, but side effects of drowsiness and confusion were common
with numbers needed to harm reported as four and nine, respectively [4].
With considerable limitations of studies with small sample sizes, short study
111
will likely be clarified as physicians become more comfortable with use but
will probably be somewhat flexible[3].
The use of antidepressant medications for pain modulation in rheumatology clinical practice, other than FM, is still preliminary. The most common
reason for caution is the concern for drug interactions, problems of tolerability in patients with other comorbidities, and especially the effect of these
agents in older patients.
112
duration, and effect sizes noted to be modest at best, any conclusions remain
tenuous and require furtherstudy.
Topical and intra-articular treatments
Although topical agents have been used to treat rheumatic pain for decades,
the resurgence of interest in the recent past deserves comment. Topical
treatments may be simple counterirritants such as menthol, NSAIDs, anesthetic agents such as ketamine, topical TCAs, and capsaicin, each with different mechanisms of action [4246]:capsaicin depletes substance P from nerve
endings after repeated application for approximately 3 weeks, counterirritants make use of gate mechanisms of pain modulation, and NSAIDs inhibit
peripheral inflammatory mediators. Prolonged cutaneous analgesia has been
demonstrated in the rat model by the application of amitriptyline, an agent
that affects sodium channels and therefore the pain response[47].
These agents provide an attractive alternative to oral treatments with
increasing evidence for effects on peripheral mechanisms of nociception and
with the added advantage of reduced systemic effects [48]. Local and systemic absorption can vary depending upon the formulation used, but generally plasma levels of drug are low, whereas local tissue concentrations can
be high [49,50]. Therefore the side-effect profile of a topical agent is more
favorable than for an orally administered treatment. Topical NSAIDs have
a better effect than placebo in management of a single joint OA or acute
muscle injuries but no effect in chronic low back pain or FM [5]. It also seems
that the analgesic effect of topical NSAIDs is apparent within the first two
weeks of treatment, with less obvious effect thereafter[52].
For the last half-century, injection of corticosteroids into bursae, tendon
sheaths, and joints has been a useful and enduring treatment strategy for
rheumatic conditions. The advantage of local injections is that the dose of
corticosteroid is modest and almost without systemic effect, success rate is
acceptable, and importantly, the risks are minimal [53,54]. The two greatest
concerns are for ()introduction of infection into a tissue space and (2)rupture of a tendon when inadvertently the tendon rather than the tendon
sheath is injected, both of which are mostly rare occurrences.
In studies of joint injections of corticosteroids, the effect is mostly of short
duration, with no evidence for long-term effect on pain or natural history of
disease [55]. In contrast, injections of corticosteroids into soft tissues structures are more efficacious in initiating prolonged improvement of symptoms
[56]. Repeated treatments may be required after several months, with anecdotal recommendations to limit the number of injections to three for each
location over a one-year period.
Intra-articular or intralesional injections may be considered as locally
applied treatments [55]. Corticosteroid are the most commonly used agent,
but with some interest in the use of botulinum toxin, or simply a local anesthetic agent. Intra-articular hyaluronic acid may have a role in the treatment of
knee OA in selected patients [57,58]. Even though hyaluronic acid is cleared
from the joint within 24 hours, the postulated mechanism of action is a
change in chondrocyte cell function and cartilage metabolism. This treatment
Otheragents
There are a number of agents, each with unique mechanisms of action,
which may have some use in pain management, although evidence in
rheumatic diseases other than FM hardly exists. The categories of drugs
included are the dopaminergic agents, NMDA receptor antagonists, and
5-hydroxytryptamine-3 receptor antagonists. Anti-Parkinsonian drugs that
augment dopamine are an effective treatment for restless legs, a frequent
accompaniment to rheumatic pain conditions. Asmall study that examined
the effect of pramipexole in FM reported improvement in symptoms of pain,
although use is tempered by frequent gastrointestinal side effects[67].
Because activation of the NMDA receptor is a mechanism by which
chronic pain is perpetuated, blockade of this receptor would be highly desirable in patients with chronic pain. However, there are no studies examining
this treatment strategy in musculoskeletal pain[68].
The 5-hydroxytryptamine-3 receptor antagonists are agents that have
been primarily used as antiemetic drugs. In a recent study of patients with
FM, dolasetron infused monthly over a period of three months resulted in
significant reduction in pain intensity compared with placebo and showed
a good safety profile [69]. Once again, there are no studies in other rheumatic pain conditions, and effects in FM must still be considered to be
preliminary.
Herbal andDiet
Herbal treatments and dietary manipulations are commonly used by patients
with rheumatic disease, mostly not prescribed by physicians and often without evidence for efficacy [60,6]. Arecent review from Japan reported that
of the 260 complementary products available for arthritis treatment in Japan,
only 4 had been tested in controlled trials [62]. In a systematic review of
the use of herbal medicine for the treatment of OA, several agents including phytodolor, capsaisin, evening primrose oil, devils claw (harpargophytum), and avocado/soya have been reported to have some effect on pain in
patients with OA [63,64]. Although studies have not reported severe side
effects, and herbal agents seem to be relatively safe, caution needs to be exercised regarding interaction with other prescribed medications.
Dietary supplementation with omega 3 polyunsaturated fatty acids (eg,
alpha linolenic acid) has been shown to possess anti-inflammatory properties and has been associated with reduction in consumption of NSAIDs in
RA [65]. Both glucosamine and chondroitin sulphate are used extensively by
patients with OA, although a recent meta-analysis indicates no reduction in
pain or joint space narrowing when compared with placebo [66]. The healthcare professional should acknowledge that disclosure by the patient of use of
complementary products speaks to a trusting doctor-patient relationship and
may even view the exploration of other treatment options as a positive effort
on the part of the patient to improve health.
113
has been shown to be effective, safe, and well tolerated, with most favorable
effects within the first three months of treatment[59].
114
Summary
The notion to consider adjuvant agent use in rheumatic conditions stems from
the knowledge of neurogenic mechanisms in FM and the overlap of FM type
pain in rheumatic disease. These agents, apart from topical applications, have
mostly not been adequately studied in rheumatic conditions, but they have
been tentatively used in clinical practice. In line with the diverse effects of some
of the adjuvant agents, with impact on sleep, mood, and even fatigue, they may
eventually be used more commonly in rheumatic diseases and not only for
treatment of FM. Benefits related to use of oral agents, especially for the older
population, need to be carefully weighed against potential risks before adjuvants can be universally recommended for routine pain management.
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117
Chapter9.4
Acute PostoperativePain
Pierre Beaulieu
Pathophysiology of postoperativepain
The etiology and treatment of pain produced by surgery are different from
other clinical pain conditions []. After in vivo neurophysiology experiments
using the rat plantar incision [0], spontaneous activity in nociceptive pathways and guarding pain were reported after incision. This postoperative model
indicates that different tissues have unique responses to incision:reducing the
amount of deep tissue injury decreases pain at rest and opioid consumption,
whereas varying the magnitude of the skin incision did not affect pain at rest
or opioid use []. Furthermore, basic science data indicate that early after
surgery, primary afferent activation and peripheral sensitization are profound
when patients postoperative pain is greatest. In addition, central sensitization
likely contributes to referred pain and secondary hyperalgesia and perhaps to
chronic posttraumatic pain[9].
119
119
Introduction
Acute PostoperativePain
Chapter9.4
120
In general, pain at rest resolves within the first week after surgery. Pain with
activities, such as coughing or walking, is severe during the first 2 to 3days
then moderate or severe for many days or even weekslater.
Management of postoperativepain
The optimal management of postoperative pain is important, not only for
humanitarian reasons (to decrease pain suffering immediately after surgery) but also because substandard acute pain management has far reaching consequences for the quality of life and consumption of healthcare
resources for a large number of patients undergoing surgical procedures
[8]. Many factors can influence the perception of postoperative pain (Table
9.4.)[38].
General management:acute pain service
Acute pain management services evolved in response to the desire for
improved management of postoperative pain. The concept of a collaborative,
interdisciplinary approach to managing postoperative pain, which included
formal education and the facilitation of clinical research in postoperative pain,
was introduced in 988 [4]. Nowadays, 90% of academic institutions have
implemented a multidisciplinary team or acute pain service[7].
Analgesics
Acetaminophen
The very low risk of acetaminophen therapy, with a highly favorable risk/benefit ratio, might justify a role for acetaminophen as a near-routine postoperative background analgesic as part of multimodal analgesia [35]. The maximal
daily dose, when used for a short period of time such as postoperative pain,
is 4 g in adults, 3 g in elderly or patients weighing less than 50kg, and 60 mg/
kg in children. An intravenous form now exists in most countries (Ofirmev
in the United States, Perfalgan in Europe) that allows an administration even
in patients nil by mouth as is often the case in the immediate postoperative
period. The administration of intravenous acetaminophen reduces the use of
other analgesics by 36%50% [43]. Furthermore, the administration of acetaminophen with opioids was associated with a morphine-sparing effect of
20% for the first 24 hours, but without any difference in side-effect profile or
patients satisfaction [37,42].
Nonsteroidal anti-inflammatorydrugs
Selective cyclooxygenase-2 antagonists (coxibs) are as effective as standard
NSAIDs in the management of postoperative pain. The administration of
NSAIDs with morphine is associated with a morphine-sparing effect of 30%
50% and with a reduction in side effects:30% less nausea and vomiting, 29%
less sedation, but no effect on the incidence of pruritus, urinary retention, or
respiratory depression [36,37].
Nonsteroidal anti-inflammatory drugs and coxibs are associated with potentially serious side effects that restrain their utilization in the postoperative
Acute PostoperativePain
Chapter9.4
Multimodal analgesia
The definition and value of multimodal or balanced analgesia in postoperative pain treatment was proposed in 993 by Kehlet and Dahl [27]. The
American Society of Anesthesiologists []defines multimodal techniques for
pain management as the administration of two or more drugs acting via different mechanisms to provide analgesia. This strategy seemed advantageous,
inasmuch as analgesic power is enhanced together with an expected gain by
reducing the risk of side effects compared with more intensive single-modality
treatment. However, the optimal combination therapy needs to be evaluated
regarding composition and duration for the various surgical procedures[27].
Today, multimodal analgesia includes the combined administration of acetaminophen, nonsteroidal anti-inflammatory drugs (NSAIDs), opioids, local
anesthetics, and, more recently, anticonvulsant analgesics, ketamine, and
possibly antidepressants. The idea behind multimodal analgesia is that combined drugs may have additive or even synergistic effects and at the same
time allows the administration of smaller doses of the drugs with potentially
more severe side effects. It is then hoped that using less opioids, for example,
will be associated with less side effects [37]. Rather than simply focusing on
the use of adjuvant analgesics for the management of postoperative pain, we
also provide a brief overview of the multimodal analgesia, including use of
acetaminophen, NSAIDs, and opioids.
121
Acute PostoperativePain
Chapter9.4
122
Gabapentinoids
Multimodal treatment of postoperative pain using analgesic anticonvulsivants
such as gabapentin or pregabalin (gabapentinoids) is becoming more common [6,7]. The anti-hyperalgesic properties of gabapentin and pregabalin
make them interesting analgesics to use in the perioperative period, to reduce
pain and opioid consumption. Chapter 4 provides more information on pharmacological and pharmacokinetic properties of gabapentin and pregabalin.
According to a recent systematic review of randomized controlled trials, postoperative pain intensity is not reduced by pregabalin [5]. However,
cumulative opioid consumption at 24 hours after surgery was significantly
decreased with pregabalin (8.8 mg reduction for doses of pregabalin <300 mg
and 3.4 mg for doses 300 mg). Pregabalin reduced opioid-related adverse
effects such as vomiting, but the risk of visual disturbance was greater.
Another recent meta-analysis on pregabalin reported that the administration of 225300 mg/day pregabalin during a short perioperative period
provides additional analgesia in the short term but at the cost of additional
adverse effects. Pregabalin increased the risk of dizziness or light-headedness
and of visual disturbances, but it decreased the occurrence of postoperative
nausea and vomiting[9].
For gabapentin, Clarke etal [3] reported that a single 600 mg dose given
preoperatively or postoperatively does not reduce morphine consumption or
pain scores in hospital or at 6months after hip arthroplasty within the context
Acute PostoperativePain
Chapter9.4
Ketamine
Ketamine, a compound with analgesic and antihyperalgesic properties, has
been shown to decrease postoperative pain and opioid requirements in adults
[4,40]. Routes of administration include intravenous, subcutaneous, epidural,
transdermal, and intra-articular. At low subanesthetic doses (0.50.5 mg/kg),
ketamine exerts a specific NMDA blockade effect and, hence, modulates
central sensitization induced both by the incision and tissue damage and by
perioperative analgesics such as opioids[47].
According to a meta-analysis [8] and a recent systematic review [29],
ketamine administered intravenously during anesthesia in adults decreases
postoperative pain intensity up to 48 hours, decreases total opioid consumption, and delays the time to first request of rescue analgesic. The greatest efficacy was found for thoracic, upper abdominal, and major orthopedic surgical
subgroups. When ketamine was effective for pain, postoperative nausea and
vomiting was less frequent in the ketaminegroup.
There is some evidence to show that perioperative administration of
low-dose ketamine might modulate the expression of OIH or analgesic tolerance and that it reduces postoperative wound hyperalgesia after acute intraoperative opioid exposure[32].
123
of small doses of ketamine, a nonselective NMDA antagonist, for its prevention or treatment. The use of multimodal analgesia is also beneficial to try
to avoid the development of OIH. It is important to note that tolerance and
OIH are pharmacologically distinct phenomena and share the same net effect
on dose requirements [3]. Amore detailed discussion of OIH and the use of
NMDA antagonists to treat postoperative pain can be found in Chapter7.
Acute PostoperativePain
Chapter9.4
124
Intra-articular catheters are also inserted within major joints (hip, knee,
shoulder) after surgery to allow the infusion of local anesthetics with good
results compared with nerve blocks [3]. The use of liposomal formulations of local anesthetics prolongs analgesic duration and is an attractive new
method of local anesthetic delivery[2].
Specific pain treatment
There is a need for the development of an evidence-based approach to
reliable, comprehensive, individualized analgesic treatment. The numberneeded-to-treat (NNT) of a particular analgesic can give a valuable overview
of efficacy, but this concept is not necessarily applicable to all types of surgery.
Table9.4.3 Comparison of Epidural Analgesia vs Opioid
Patient-Controlled Analgesia (from[6])
Pain control
atrest
on mobilization
Side effects
hypotension
postoperativeileus
nausea/vomiting
urinary retention
sedation
Reduction in postoperative morbidity
cardiovascular
respiratory
nurses workload
Epidural
Analgesia (Local
Anesthetics)
Opioid
Patient-Controlled
Analgesia
+++
++
++
shortening
+
prolongation
++
+
+
+
+
+
125
Chapter9.4
Neuroaxial blocks
epidural
spinal
combined spinal/epidural
caudal
Peripheral nerve and plexus blocks
plexus blocks:brachial and lumbosacral
proximal and distal nerves
intercostal
paravertebral
transversus abdominis plane block
Incisional blocks:subcutaneous, subfascial
Intraarticular and intrabursal blocks
Acute PostoperativePain
Acute PostoperativePain
Chapter9.4
126
650mg
g
Route of
Administration
Oral
Intravenous
Frequency of
Administration
4hourly
6 hourly
Acetaminophen
500mg
00 mg
Oral
Oral
2hourly
2 hourly
600mg
300 mg
Oral
Oral
h preoperatively
h preoperatively
37.5mg
Oral
duloxetine
60 mg
Oral
Ketamine
0.5mg/kg
05g/kg
per min
Maximaldose
23mg/kg
23mg/kg
2 mg/kg
Intravenous
Continuous
intravenous infusion
Subcutaneous,
subfascial, topical,
epidural, perineural,
intraarticular
Nonsteroidal
anti-inflammatory drugs
naproxen
celecoxib
Gabapentinoids
gabapentin
pregabalin
Antidepressants*
venlafaxine
Local anesthetics
bupivacaine
levobupivacaine
ropivacaine
4 hourly
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Chapter0
Drug-Drug Interactions of
Adjuvant Analgesics
David R.P.Guay
Drugs can interact with other drugs, excipients in the dosage formulation,
components of large-volume parenteral solutions, foodstuffs, nutrients, etc.
For purposes of this chapter, only drug-drug interactions will be presented.
Drug-drug interactions can affect the pharmacokinetics (ie, absorption, distribution, metabolism, and excretion) or pharmacodynamics (ie, responses
good and bad) of one or both drugs involved. An adverse reaction may, in
turn, result. The severity of drug-drug interactions is influenced by several
factors including the therapeutic indices of the drugs (ie, the ratio of toxic
to therapeutic concentrations or doses), age-related changes in physiology
applicable to the mechanism of the interaction, drug doses, and, in some
cases, pharmacogenetics. Pharmacogenetics, as applied to drug-drug interactions, centers around genetic-based differences in drug metabolism (eg,
poor vs extensive metabolizers of specific cytochrome P450 isozymes). This
chapter will present drug-drug interactions of adjuvant analgesics with other
adjuvant analgesics or drugs of other classes.
131
131
Introduction
132
Chapter0
Drug-drug Interactions
Other Adjuvant
SSRIs, SNRIs
Interactions
serotonergic effects
Mechanism
Additive serotonergic effects at
synapse
Inhibition of TCA drug metabolism
by SSRIs/SNRIs (inhibition of
CYP450 isosymes 2D6, A2, 2C9,
2C9, 3A4. Note:range of number
of isozymes inhibited and potency
of inhibition vary between SSRIs)
TCA (parent +/ active
metabolite) serum concentrations
serotonergic effects at synapse
Evidence
Reportedwith
Amitriptyline + sertraline
Imipramine/desipramine +
fluvoxamine
Clomipramine + fluvoxamine
TCAs + fluvoxamine
TCAs + venlafaxine
TCAs []
Phenytoin
plasma phenytoin
concentrations
Unknown
CBZ [2]
Valproate
Variable effects
on plasma CBZ
concentrations
plasma CBZ epoxide
concentrations
plasma valproate
concentrations
Recommendations
Avoid this combination
if possible
If must use a TCA,
avoid clomipramine
as it is the most
serotonergicTCA
If must use a SSRI,
use citalopram or
escitalopram because
these interact least with
CYP450 isozymes
Use TCA other than
imipramine
Careful monitoring of
toxicity/loss of efficacy
and therapeutic drug
monitoring are necessary
whenever regimen of
either agent is altered
CBZ [2,3]
Phenytoin
plasma CBZ
concentrations
Variable effect on
plasma phenytoin
concentrations
Pharmacokinetic studies
CBZ [2,4]
Lamotrigine
lamotrigine plasma
concentration
CBZ epoxide plasma
concentrations
Caseseries
Pharmacokinetic studies
CBZ [,
2,5]
TCAs
plasma TCA
concentrations
Induction of TCA
CYP450-mediated metabolism by
CBZ
Careful monitoring of
toxicity/loss of efficacy
and therapeutic drug
monitoring are necessary
whenever regimen of
either agent is altered
Careful monitoring of
toxicity/loss of efficacy
and therapeutic drug
monitoring are necessary
whenever regimen of
either agent is altered
Avoid combination if
possible.
Monitor carefully if CBZ
regimen is changed.
May require therapeutic
drug monitoring of
bothdrugs.
Beware TCA toxicity if
CBZ dose is reduced or
CBZ therapy is stopped
without a reduction in
TCA dose.
(continued)
133
Chapter0
Drug-drug Interactions
134
Chapter0
Drug-drug Interactions
Table0.Continued
Interactions
Mechanism
Lamotrigine Phenytoin
[6]
Adjuvant
Other Adjuvant
lamotrigine plasma
concentrations
TCA [7]
plasma TCA
concentrations
Venlafaxine
Duloxetine
Evidence
Pharmacokinetic studies
Recommendations
Dramatic lamotrigine
concentration is
unlikely
Following lamotrigine
plasma concentrations
during phenytoin
dose titration and
subsequent phenytoin
dose adjustments is
reasonable
Avoid the combination
by substituting an SSRI
with minimal CYP450
isozyme 2D6inhibiting
potential (eg. citalopram)
for venlafaxine/duloxetine
and/or substituting a
TCA not dependent on
CYP450 isozyme 2D6 for
its metabolism(eg,
nortriptyline).
Abbreviations:CBZ, carbamazepine; SNRIs, serotonin norepinephrine reuptake inhibitors; SSRIs, selective serotonin reuptake inhibitors; TCAs, tricyclic antidepressants.
TCAs [9,0]
CBZ []
Methadone
Mechanism
Evidence
ASA unbound (free)
One case series
plasma concentrations via
plasma protein displacement
Unknown. Possible
additive/synergistic
antiplatelet effects of TCAs
and NSAIDs
Recommendations
Transient effect, so monitor for adverse
effects of imipramine at initiation of ASA
Population-based,
Replace TCA by another antidepressant
case-cohort study
with minimal or no serotonergic
reported bleeding
activityor
risk; however, lower
Replace NSAID by nonacetylated
than with SSRI-NSAID
salicylate, celecoxib or acetaminophen
combinations
If must use a TCA and NSAID,
Another study did not
use desipramine, trimipramine, or
observe interaction
nortriptyline because these are
minimally serotonergic
Case series of patients Avoid combination if possible
on methadone
If not possible, careful monitoring when
maintenance therapy
dose of CBZ is altered
who experienced
Monitor for necessary adjustment
opioid withdrawal
of methadone dose after CBZ
symptoms after
discontinuation
introductionofCBZ
Case report of
methadone-associated
respiratory depression
after discontinuation
ofCBZ
(continued)
135
Chapter0
Drug-drug Interactions
136
Chapter0
Drug-drug Interactions
Table0.2Continued
Adjuvant
CBZ [2]
Lamotrigine [3]
Acetaminophen
lamotrigine plasma
concentrations
with initiation of
acetaminophen
Corticosteroids
[4]
Phenytoin
plasma
corticosteroid
and phenytoin
concentrations
Mechanism
N-demethylation
pathways of codeine by
hepatic enzyme-inducing
effects of CBZ
urinary excretion of
norcodeine while urinary
excretion of normorphine
is unchanged
Unknown
Evidence
Case series of
epileptic patients
Recommendations
Clinical relevance unknown
Pharmacokinetic
studies in eight
healthy volunteers
Phenytoin-associated
Caseseries
enhancement of
Pharmacokinetic
corticosteroid metabolism
studies
(eg, 6--hydroxylation)and
Corticosteroid-associated
enhancement of
phenytoin metabolism
(primarily seen with
dexamethasone).
Prednisone
NSAIDs
incidence/severity
Additive gastrointestinal
of NSAID-associated
mucosal injury
and/or corticosteroidassociated peptic ulcer
disease, gastritis, etc
Theoretical
interaction. Few data
available
Duloxetine
Venlafaxine
SSRIs [9, 0,
5,6]
NSAIDs
risk of upper
gastrointestinal
bleeding
Unknown
Possibly additive platelet
function inhibition
Bisphosphonates
(oral only)
[7,8]
NSAIDs
Large
population-based,
cohortstudy
Nested
case-controlstudy
Meta-analysis of
observational studies
Open-label study in
26 healthy volunteers
Retrospective
case-control study did
not find interaction
137
Chapter0
Drug-drug Interactions
138
Chapter0
Drug-drug Interactions
Table0.2Continued
Adjuvant
Serotonergic
antidepressant
(SSRIs,
venlafaxine,
mirtazapine,
trazodone,
imipramine,
clomipramine)
Paroxetine and
other inhibitors
of CYP2D6[27]
tramadol efficacy
Mechanism
Additive effects
on serotonergic
neurotransmission
Evidence
Several case reports,
including lethal
interaction
Recommendations
Substitute a minimal or nonserotonergic
antidepressant and/or nonserotonergic
analgesic.
generation of active
O-desmethyl metabolite
pharmacokinetic
studies
Use antidepressant
that does not inhibit CYP2D6
Abbreviations:ASA, aspirin; CBZ, carbamazepine; NSAIDs, nonsteroidal anti-inflammatory drugs; SNRIs, serotonin norepinephrine reuptake inhibitors; SSRIs, selective serotonin reuptake
inhibitors; TCA, tricyclic antidepressants.
Stimulation of Stimulation
5-HT Releaseb of 5-HT
Synthesis
SSRIs
Inhibition
Stimulation of
of 5-HT
Postsynaptic
Metabolism Receptor
Pathway
MAOIs
Carbamazepine
Fluoxetine
Moclobemide Lithium
Paroxetine
Selegiline
5-HT agonists
MDMA
(ecstacy)
Fenfluramine
Sertraline
Rasagiline
Sumatriptan
Cocaine
Fluvoxamine
Tranylcy
promine
Phenelzine
MAOIs
St. Johns
Wort
Selegiline
Citalopram
SNRIs
Amphetamine
5-Hydroxy
tryptophan
L-tryptophan
Chapter0
Inhibition
of 5-HT
Releasea
Drug-drug Interactions
Moclobemide
Venlafaxine
Rasagilinec
Duloxetine
Tranylcypromine
TCAs
Phenelzine
139
Amitriptyline
Imipramine
Clomipramine
Doxepin
Desipramine
Other ADs
Trazodone
Nefazodone
Opioids
Tramadol
Tapentadolc
Meperidine
Methadone
Fentanyld
Dextrome
thorphan
(continued)
Drug-drug Interactions
Table0.3Continued
Chapter0
Cocaine
Inhibition
of 5-HT
Releasea
Inhibition
Stimulation of
of 5-HT
Postsynaptic
Metabolism Receptor
Pathway
Stimulation of Stimulation
5-HT Releaseb of 5-HT
Synthesis
Others
Amphetamine
St. Johns
Wort
Abbreviations:ADs, antidepressants; 5-HT, serotonin; MAOIs, monoamine oxidase inhibitors;
MDMA, methylenedioxymethamphetamine; SSRI, selective serotonin reuptake inhibitor; SNRIs,
serotonin norepinephrine reuptake inhibitors; TCAs, tricyclic antidepressants.
a
From synapse.
140
Drug-drug Interactions
Chapter0
141
periods of risk, even after drug cessation, of serotonin excess should another
serotonin-active drug be started. This is also why the addition of a drug inhibiting the metabolism of a serotonin-active drug may actually precipitate serotonin toxicity. There are many agents that can inhibit one or more isozymes
of the cytochrome P450 family of drug-metabolizing enzymes. Addition of
one of these enzyme inhibitors will lead to a reduction in metabolism of the
other (serotonergic) drug, causing drug accumulation until serotonin toxicity supervenes. In other cases, enzyme inhibition will lead to a reduction in
analgesic effect if it results in reduced generation of an active metabolite (eg,
tramadol, codeine). In other cases, the addition of an enzyme stimulant
may lead to enhanced drug metabolism and a reduction in drug (ie, analgesic)
response [28]. More details regarding serotonin toxicity are available in the
relevant sections of Tables0. and0.2.
A survey was conducted in Australia of deaths from 2002 to 2008, wherein
one or more of the following serotonergic drugs were found at autopsy:tramadol, venlafaxine, fluoxetine, sertraline, citalopram, paroxetine, and MDMA
(ecstasy). Although 23 such deaths were found, in 28 cases there were
signs or symptoms antemortem, which was suggestive of serotonin syndrome and believed to have contributed to the subjects death. In cases,
two or more potential analgesic agents were found. Tramadol and venlafaxine
were involved in six cases each. Among the six venlafaxine recipients, five and
one subject had venlafaxine plus an opioid (tramadol in one, methadone in
four) and venlafaxine plus a tricyclic antidepressant (amitriptyline) present,
respectively. In addition, the relative prevalences of these serotonergic agents
in the 23 cases were calculated by adjusting for annual drug consumption of these agents in Australia over the 20022008 data collection period.
Tramadol scored 0.5 followed by ecstasy (4.57), fluoxetine (3.02), and the
remainder (.47). The data from this report substantiate the lethal potential
for serotonergic combinations, especially those involving either tramadol or
venlafaxine[9].
There are striking similarities between tramadol and venlafaxine that
may explain the findings just described. First, the structural similarities
are great:each has methoxyphenyl, N,N-dimethylamino, and hydroxycyclohexyl groups (groups may assume near-superimposable intermolecular orientations). Second, they have the same prominent adverse effects
(nausea, headache, dizziness). Third, both inhibit the reuptake of serotonin
and norepinephrine. Fourth, both undergo enantioselective metabolism via
CYP450 isozyme 2D6. Finally, both are metabolized to active desmethyl
metabolites.
142
Chapter0
Drug-drug Interactions
Gingko [32]
Gingko [33]
St. Johns
Wort [34]
St. Johns
Wort [35]
St. Johns
Wort [36]
Analgesic
Interactions
Acetaminophen exposure to acetaminophen and its
glucuronide metabolite
NSAIDs
Possible bleeding risk
Recommendations
Unlikely to be clinically
significant
Theoretical assumption without clinical Likely clinically relevant
Garlic platelet
only with excessive
aggregation as do data of effect of combination of
garlic-NSAIDs on bleeding risk
doses of garlic
NSAIDs
Aspirin
No additive effects occur for the combination
Randomized controlled trial
No interaction
of ginkgo300mg
daily and aspirin 325 mg daily over 2 weeks in
terms of clotting time or platelet aggregation.
Ibuprofen
One case report of fatal intracerebral No clear evidence of
Possible bleeding risk
bleed
interaction
Anticonvulsants plasma concentrations of anticonvulsants
CYP2C9
One case report of fatal seizure in one No clear evidence of
metabolised by
induction by
patient on stable doses of phenytoin
interaction
CYP2C9
gingko
and valproate who started gingko
Amitriptyline
Induction of
Crossover trial evaluating plasma
Monitor therapeutic
systemic exposure to amitriptyline and its
CYP3A4 and/or concentrations of amitriptyline and
response
active metabolite nortriptyline
P-gp by St.Johns nortriptyline with/without concurrent
Wort
St. Johns Wort
Venlafaxine
Precipitation of serotonin syndrome
Unknown.
Case report of serotonin syndrome
No clear interaction or
No causality
in patient on venlafaxine who started
causality
established.
St. Johns Wort, resolved after
discontinuation
Methadone
Induction of
Pharmacokinetic study in 4 patients
Monitor therapeutic
plasma concentrations of methadone
CYP3A4 and/or
response. Beware
P-gp by St.Johns
opioid withdrawal
Wort
signs/symptoms
Mechanism
Unknown
Evidence
Pharmacokinetic study
References
. Gilman PK. Tricyclic antidepressant pharmacology and therapeutics:drug interactions updated. Br J Pharmacol 2007; 5:737748.
2. Ramsey RE, McManus DQ, Gutterman A, etal. Carbamazepine metabolism in
humans:effect of concurrent anticonvulsant therapy. Ther Drug Monit 990;
2:23524.
3. Browne TR, Szabo GK, Evans JE, etal. Carbamazepine increases phenytoin
serum concentration and reduces phenytoin clearance. Neurology 988;
38:4650.
4. Malminiemi K, Keranen T, Kerrtula T, etal. Effects of short-term lamotrigine
treatment on pharmacokinetics of carbamazepine. Int J Clin Pharmacol Ther
2000; 38:540545.
5. Leinonen E, Lillsunde P, Laukkanen V, Ylitalo P. Effects of carbamazepine on serum antidepressant concentrations in psychiatric patients. J Clin
Psychopharmacol 99; :3338.
Drug-drug Interactions
Chapter0
Summary
143
Drug-drug Interactions
Chapter0
144
Drug-drug Interactions
Chapter0
145
Index
A
Acetaminophen, 9t
adverse effects and side
effects of, 3
dosage and administration
of, 3, 2
garlic and, interactions
between, 42t
indications for, 3, 6, 6t, 8t
intravenous, 2
lamotrigine and, drug-drug
interactions, 36t
liver toxicity of, 3
in multimodal analgesia,
2
and opioids, combination
therapy with, 2
for postoperative pain, 2
dosage and
administration of,
27t
Acute pain service, 20
Adjuvant analgesic(s)
for bone pain, 7, 7t
for bowel obstruction,
7, 7t
classification of, by clinical
efficacy, 7, 7t
definition of, 5
multipurpose, 7, 7t
for musculoskeletal pain,
7, 7t
for neuropathic pain, 7, 7t
and other analgesics,
drug-drug
interactions,
35t38t
on WHO analgesic/pain
ladder, 2, 2f, 6, 6t
Adjuvant drug(s), definition
of, 5
Adjuvant medicine(s),
definition of, 5
2-Adrenergic agonists, 7t
adverse effects and side
effects of, 00
for cancer pain, 96t,
9900
dosage and administration
of, 99t
mechanism of action
of, 0t
-Adrenergic receptor(s),
as drug targets, 9t
2-Adrenergic receptor(s),
as drug targets, 9t
Allergic reaction(s), 6, 8
to local anesthetic, 55
to methylparabene, 55
Allodynia, , 79
definition of, 5960
intraoperative opioids
and, 606
Amantadine
for cancer pain, 96t
for cancer-related
neuropathic pain,
02
mechanism of action
of, 63
American Society of
Anesthesiologists,
guidelines for acute
pain management
in perioperative
setting, 9, 26
Amitriptyline,
adverse effects and side
effects of, 2t, 8t
for arthritis pain, 6
for cancer pain, 88, 96t,
9798
dosage and administration
of, 2t, 8, 80, 8t
efficacy of, 4
for fibromyalgia, 5, 7,
0
half-life of, 2t
for headache, 57
for low back pain, 6
mechanism of action
of, 8t
for neuropathic pain, 4,
7, 80, 8t, 88
placebo-controlled
trials of, 3t
neurotransmitter profile
of, 2t
for postmastectomy
pain, 88
precautions with, 8t
St. John's wort and,
interactions
between, 42t
and serotonergic activity,
39t
and sertraline, drug-drug
interactions, 32t
topical, 2
venlafaxine and, drug-drug
interactions, 4
Amphetamines, and
serotonergic
activity, 39t40t
Analgesic(s)
classification of
by clinical efficacy, 5,
6t, 7, 7t
mechanistic approaches
for, 5, 6t, 78,
8t9t
by pain severity, 56, 6t
by therapeutic class,
5, 6t, 7
mechanistic taxonomy of,
8, 9t0t
multipurpose, for cancer
pain, 9596, 96t,
9700, 99t
serotonergic, 34,
39t
topical. See Topical
analgesics
Anandamide, 35f
Ankylosing spondylitis, pain
of, treatment
of, 6
Anorexia, AIDS-related,
cannabinoids
for, 34t
Antiarrhythmics, 7
drug interactions with, 8
Antibiotic(s), drug
interactions with,
8
Anticholinergics, 7t
for cancer pain, 97t
dosage and
administration
of, 99t
147
Index
148
Anticholinergics (Cont.)
for cancer-related bowel
obstruction, 03
Anticonvulsant(s), 57. See
also specific drug
analgesic efficacy of, 2
for cancer pain, 96t
for fibromyalgia, 080,
09t
indications for, 8t
mechanism of action
of, 2
for neuropathic pain, 86
cancer-related, 0
for rheumatic pain, 09t
Antidepressant(s), 57, 7t. See
also specific drug
adverse effects and side
effects of, 2t, 6
analgesic effects of,
mechanism of
action of, 34
anti-inflammatory effects
of, 0
baseline tests with, 8
for cancer pain, 96t,
9798, 99t
for chronic noncancer pain
randomized controlled
trials of, 7
selection of, 67
in combination therapy, 9
contraindications to,
78
dosage and administration
of, 89
drug interactions with, 8
for fibromyalgia, 5, 08,
09t
for headache, 56
indications for, 8t
for low back pain, 6
mechanism of action of,
0
monitoring of therapy
with, 89
for neuropathic pain,
45
cancer-related, 0
patient education about,
8
for postoperative pain,
24
dosage and
administration of,
27t
precautions with,
for rheumatic pain, 09t,
0
serotonergic
and methadone,
drug-drug
interactions, 38t
and tapentadol,
drug-drug
interactions, 38t
and tramadol,
drug-drug
interactions, 38t
Antifungals, drug interactions
with, 8
Antihyperalgesics, 9t
Antinociceptive analgesics, 9t
and modulators of
descending
inhibition/
excitation,
mixed, 0t
Anti-Parkinsonian drugs, 3
Antipsychotics, drug
interactions with,
8
Antiretrovirals, drug
interactions with,
8
Antispasmodics, indications
for, 8t
Anxiety, improvement
drugs for, 8t82t
mirtazapine for, 98
Arrhythmia(s), local
anestheticinduced, 5355
Arthritis pain, . See also
Inflammatory
arthritis;
Osteoarthritis;
Rheumatoid
arthritis (RA)
treatment of, 67
Atropine, for cancer pain,
97t
B
Baclofen, 7t
for cancer pain, 97t
for cancer-related
neuropathic pain,
02
Bisphosphonates, 56, 7t
adverse effects and
side effects of,
0203
for cancer pain, 97t
for cancer-related bone
pain, 0203
mechanism of action of,
0t, 02
oral
and multivalent
cations, drug-drug
interactions, 43
and NSAIDs, drug-drug
interactions, 37t,
43
precautions with,
0203
Bone pain
adjuvant analgesics for,
7, 7t
cancer-related
analgesics used for, 97t
bisphosphonates for,
0203
calcitonin for, 97t, 03
dosage and
administration
of, 99t
clodronate for,
0203
corticosteroids for,
9899
ibandronate for,
0203
monoclonal antibody
for, 0203
osteoclast inhibitor for,
0203
pamidronate for,
0203
radiopharmaceuticals
for, 97t, 03
samarium-53 for, 97t,
03
strontium-89 for, 97t,
03
treatment of, 0203
zolendronate for,
0203
treatment of, 7, 7t
Botulinum toxin type A
for neuropathic pain, 89
for rheumatic pain, 2
Bowel obstruction pain
analgesics used for, 97t
dosage and
administration
of, 99t
cancer-related
analgesics used for, 97t
corticosteroids for,
9899
treatment of, 0304
treatment of, 7, 7t
Bupivacaine, 52
analgesic potency of, 52t
duration of action, 52t
maximum daily dose
of, 55t
molecular structure of,
505, 5f
onset of action, 52t
pharmacology of, 50,
52t, 54f
for postoperative pain,
dosage and
administration
of, 27t
C
Calcitonin, 7t
for cancer-related bone
pain, 97t, 03
dosage and
administration
of, 99t
mechanism of action
of, 0t
Calcium channel 2d ligands
adverse effects and side
effects of, 82t
dosage and administration
of, 82t, 84
mechanism of action of,
82t, 84
for neuropathic pain,
82t, 84
precautions with, 82t
Calcium-channel blockers,
drug interactions
with, 8
Calcium channels, N-type, as
drug targets, 9t
Camphor, 76
Cancer pain
adjuvant analgesics
used for, 9596,
96t97t
2-adrenergic agonists for,
96t, 9900
dosage and
administration
of, 99t
amantadine for, 96t
amitriptyline for, 88, 96t,
9798
anticholinergics for, 97t
dosage and
administration
of, 99t
anticonvulsants for, 96t
antidepressants for, 96t,
9798, 99t
atropine for, 97t
baclofen for, 97t
bisphosphonates for, 97t
bupropion for, 96t, 98
cannabinoids for, 34t, 39,
96t, 00
dosage and
administration
of, 00
carbamazepine for, 96t
citalopram for, 96t
clonazepam for, 97t
Index
149
Bupropion
for cancer pain, 96t, 98
contraindications to, 6
for neuropathic pain, 4
Bursa block, 48t
Index
150
Cannabinoids (Cont.)
analgesic efficacy of,
4042
antispasmodic effects of,
3738
anxiolytic effects of, 37
available for medical
practice, 33, 34t
for cancer pain, 34t, 39,
96t, 00
dosage and
administration
of, 00
for chronic pain, 34t,
3639
dependence, 40, 4t, 90
for fibromyalgia, 3839,
09t,
for HIV-related
neuropathy,
3637
indications for, 8t
mechanism of action of,
for HIV-related
neuropathy,
83t, 88
for neuropathic pain,
7, 83t, 8586
topical, 7576
adverse effects and
side effects of,
7576, 86
for cancer pain, 96t,
00
in combination therapy,
76
for HIV-related
neuropathy,
7576, 8586
for rheumatic pain,
09t, 2
Carbamazepine, 23, 86
adverse effects and side
effects of, 23, 24t
analgesic efficacy of, 2
for cancer pain, 96t
and codeine, drug-drug
interactions, 36t
contraindications to, 24t
dosage and administration
of, 24t
and lamotrigine, drug-drug
interactions, 33t
mechanism of action of,
0t, 24t
and methadone,
drug-drug
interactions, 35t
molecular target of, 9t
and phenytoin, drug-drug
interactions, 33t
precautions with, 24t
and serotonergic activity,
39t
and TCAs, drug-drug
interactions, 33t
for trigeminal neuralgia,
23, 86
and valproate, drug-drug
interactions, 32t
Cardiac arrest, local
anestheticinduced, 5355
Catastrophizing, and
neuropathic
pain, 90
Cauda equina syndrome,
local anestheticinduced, 5355
Causalgia, 8t
Celecoxib, for postoperative
pain, dosage and
administration of,
27t
Central sensitization, 8,
9t, 9
D
Denosumab, for prevention
of skeletal
complications in
prostate cancer,
03
Depression
drugs for, 8t. See also
Antidepressant(s)
mirtazapine for, 98
Desipramine,
adverse effects and side
effects of, 2t, 8t
for cancer pain, 96t,
9798
dosage and administration
of, 2t, 8t
efficacy of, 4
and fluvoxamine,
drug-drug
interactions, 32t
half-life of, 2t
mechanism of action
of, 8t
for neuropathic pain,
4, 8t
placebo-controlled
trials of, 3t
neurotransmitter profile
of, 2t
precautions with, 8t
and serotonergic activity,
39t
Desvenlafaxine, for cancer
pain, 96t
Dexamethasone
for cancer pain, 96t,
9899
dosage and
administration of,
99, 99t
for pain emergencies, 99
Dextromethorphan, 63
for cancer pain, 96t
for cancer-related
neuropathic pain,
02
molecular target of, 9t
and serotonergic activity,
39t
Diabetic neuropathy, painful,
45, 7, 7986
combination therapy
for, 89
duloxetine for, 8t
gabapentin for, 22, 82t
opioid agonists for, 83t,
85
pregabalin for, 22, 82t
topical capsaicin for,
7576
topical lidocaine for, 74
tramadol for, 83t, 84
treatment of, 2223, 27,
86, 8889
tricyclic antidepressants
for, 8t
venlafaxine for, 8t
Diarrhea, drugs causing, 2t
Diclofenac
mechanism of action of, 72
patch, 72
topical
adverse effects and side
effects of, 7273
gel, 72
randomized
controlled trials
of, 7274, 73t
solution, with DMSO,
72
randomized
controlled trials
of, 7274, 73t
Dietary therapy, for
rheumatic pain,
3
Divalproex. See also Sodium
divalproex
Index
151
for cancer-related
neuropathic pain,
02
Clonidine
adverse effects and side
effects of, 00
for cancer pain, 96t,
9900
molecular target of, 9t
Coanalgesics, 6
definition of, 5
Cocaine
maximum daily dose
of, 55t
pharmacology of, 50
and serotonergic activity,
39t40t
Codeine, 6, 6t
carbamazepine and,
drug-drug
interactions, 36t
Coeliac block, 2
Cognitive-behavioral
therapy,
Complementary and
alternative
medicine (CAM)
and analgesics,
interactions
between,
443, 42t
for rheumatic disease, 3
Complex regional pain
syndrome,
treatment of, 22
Constipation, drugs causing,
2t, 8
Corticosteroid(s), 7t
adverse effects and side
effects of, 98
for cancer pain, 96t97t,
9899
dosage and
administration of,
99, 99t
intra-articular injections,
2
intralesional injections,
2
joint injections, 2
local injection, for
rheumatic pain,
2
and opioids, combination
therapy with, 98
and phenytoin,
drug-drug
interactions, 36t
soft-tissue injections, 2
Counterirritants
mechanism of action of,
2
for rheumatic pain, 2
Index
152
Divalproex (Cont.)
for cancer pain, 96t
Dolasetron, for fibromyalgia,
3
Dopaminergic agents, 3
Douleur Neuropathique
en 4 questions
(DN4), 79
Doxepin
adverse effects and side
effects of, 2t
dosage and administration
of, 2t
half-life of, 2t
for low back pain, 6
neurotransmitter profile
of, 2t
and serotonergic activity,
39t
Dronabinol, 36
for cancer pain, 39, 96t,
00
for chronic pain, 40
dosage and administration
of, 34t
for fibromyalgia, 38
indications for, 34t
for MS-associated pain, 38
Drowsiness, drugs causing, 8
Drug-drug interactions. See
also specific drug
between adjuvant
analgesics, 3,
32t34t
and other analgesics,
35t38t
with antidepressants, 8
between herbals and
analgesics,
443, 42t
pharmacogenetics of, 3
severity of, factors
affecting, 3
Dry mouth, drugs causing,
2t, 8
Duloxetine, 5,
adverse effects and side
effects of, 2t, 8t
for cancer pain, 96t
for central neuropathic
pain, 88
dosage and administration
of, 2t, 80, 8t,
0
for fibromyalgia, 5, 7,
07, 09t
half-life of, 2t
for low back pain, 07,
0
mechanism of action
of, 8t
for neuropathic pain, 4,
7, 8084, 8t, 86
neurotransmitter profile
of, 2t
and NSAIDs, drug-drug
interactions, 37t,
43
for osteoarthritis pain,
07
and other serotonergic
agents, drug-drug
interactions, 43
for oxaliplatin-induced
peripheral
neuropathy, 98
for postoperative pain,
dosage and
administration of,
27t
precautions with, 8t
and serotonergic
activity, 39t
and serotonin
syndrome, 40
E
Ecstasy (drug)
and serotonergic activity,
39t
and serotonin syndrome,
4
Ectopic discharge, 8, 9t
Effexor. See Venlafaxine
Endocannabinoid system,
3336, 35f
Epidural block, 3, 24, 25t
and patient-controlled
analgesia,
comparison of,
24, 25t
Escitalopram, for neuropathic
pain, 4
Etidocaine
analgesic potency of, 52t
duration of action, 52t
onset of action, 52t
pharmacology of, 52t
Eucalyptol, 76
European Society of Regional
Anaesthesia, 26
Excitation, descending,
modulators of, 9t
Exercise, in pan
management,
F
Facial pain, 4
Failed back syndrome, 88
Felbamate, 28
Femoral nerve block, 4849
Fenfluramine, and
serotonergic
activity, 39t
Fentanyl
indications for, 6, 6t
intranasal administration
of, 22
and other serotonergic
agents, drug-drug
interactions, 43
in patient-controlled
analgesia, 22
and serotonergic activity,
39t
Fibromyalgia, 8t, , 4
amitriptyline for, 5, 7,
0
anticonvulsants for,
080, 09t
antidepressants for, 5,
08, 09t
cannabinoids for, 3839,
09t,
citalopram for, 5
dolasetron for, 3
dronabinol for, 38
duloxetine for, 5, 7,
07, 09t
fluoxetine for, 5
gabapentin for, 22,
080, 09t
gabapentinoids for,
080
milnacipran for, 5, 7,
07, 09t
moclobemide for, 5, 7
monoamine oxidase
inhibitors
(MAOIs) for,
5, 7
nabilone for, 38, 09t,
nortriptyline for, 0
paroxetine for, 5
pathophysiology of,
0708
pirindole for, 5, 7
pramipexole for, 3
pregabalin for, 2223,
070, 09t
SNRIs for, 5, 7, 09t,
0
SSRIs for, 5, 7, 09t
treatment of, 5, 7,
223, 27, 07
tricyclic antidepressants
for, 7, 09t, 0
Flecainide, 49
Fluoxetine
anti-inflammatory effects
of, 0
for fibromyalgia, 5
and serotonergic activity,
39t
and serotonin syndrome,
404
G
Gabapentin, 223, 74
adverse effects and side
effects of, 23, 82t
analgesic efficacy of, 2
for cancer pain, 96t
for chronic noncancer
pain, 7
for diabetic neuropathy,
22, 82t
dosage and administration
of, 222, 82t, 84
perioperative, 24
and EMLA cream,
combination
therapy with, for
neuropathic pain,
cancer-related, 0
for fibromyalgia, 22,
080, 09t
gastroretentive
formulation of, 22
adverse effects and side
effects of, 24t
contraindications to,
24t
dosage and
administration of,
22, 24t
mechanism of action
of, 24t
for postherpetic
neuralgia, 22
precautions with, 24t
and imipramine,
combination
therapy with, for
cancer-related
neuropathic pain,
0
immediate-release
adverse effects and side
effects of, 24t
contraindications to,
24t
H
Headache,
cancer-related,
corticosteroids
for, 9899
treatment of, 57
Index
dosage and
administration
of, 24t
mechanism of action
of, 24t
precautions with, 24t
indications for, 22
mechanism of action of,
2, 82t, 84
molecular target of, 9t
and morphine, combination
therapy with,
for neuropathic
pain, 89
for neuropathic pain, 5,
7, 2223, 82t,
84, 86, 8889
cancer-related, 0
in hemodialysis
patients, 23
and nortriptyline,
combination
therapy with, for
neuropathic pain,
8889
and opioids, combination
therapy with, for
cancer-related
neuropathic pain,
0
and oxycodone,
combination
therapy with,
for neuropathic
pain, 89
pharmacology of, 222
for postherpetic neuralgia,
22, 82t
for postoperative pain,
2324
dosage and
administration of,
27t
precautions with, 82t
for spinal cord
injury-related pain,
82t, 8688
Gabapentin enacarbil, 22
adverse effects and side
effects of, 24t
contraindications to, 24t
dosage and administration
of, 22, 24t
mechanism of action
of, 24t
precautions with, 24t
Gabapentinoids, 5, 7t, 9t,
3, 223
adverse effects and side
effects of, 0
analgesic efficacy of, 2
for chronic noncancer
pain, 7
153
Fluvoxamine
clomipramine and,
drug-drug
interactions, 32t
desipramine and,
drug-drug
interactions, 32t
imipramine and,
drug-drug
interactions, 32t
and serotonergic activity,
39t
tricyclic antidepressants
and, drug-drug
interactions, 32t,
34t
Index
154
Hemodialysis patient(s),
peripheral
neuropathy in,
treatment of, 23
Herbal therapy
and analgesics,
interactions
between,
443, 42t
for rheumatic pain, 3
Herpes zoster, acute,
treatment of, 22
Human immunodeficiency
virus (HIV)
neuropathy, 45
cannabinoids for, 3637
capsaicin patch for, 83t
topical capsaicin for,
7576, 8586
treatment of, 22, 27, 88
Hyaluronic acid,
intra-articular
injections, for
osteoarthritis in
knee, 23
Hydrocodone, indications
for, 6, 6t
Hydromorphone
indications for, 6, 6t
in patient-controlled
analgesia, 22
5-Hydroxytryptophan, and
serotonergic
activity, 39t
5-Hydroxytryptophan-
receptor
antagonists, and
serotonergic
activity, 39t
5-Hydroxytryptophan-3
receptor
antagonists, 3
Hyperalgesia, 79
definition of, 5960
intraoperative opioids
and, 606
opioid-induced, 606,
6f, 85, 2223
postoperative, 60
prevention, ketamine
and, 23
primary, 59
secondary, 9
Hyponatremia,
oxcarbazepineinduced, 25t
I
Ibandronate
for cancer pain, 97t
for cancer-related bone
pain, 0203
ID Pain, 79
Imipramine
adverse effects and side
effects of, 2t
for arthritis pain, 6
and aspirin, drug-drug
interactions, 35t
dosage and administration
of, 2t
and fluvoxamine,
drug-drug
interactions, 32t
half-life of, 2t
and methadone,
drug-drug
interactions, 38t
for neuropathic pain,
4, 88
placebo-controlled
trials of, 3t
neurotransmitter profile
of, 2t
and phenytoin, drug-drug
interactions, 32t
and serotonergic activity,
39t
and tapentadol, drug-drug
interactions, 38t
and tramadol, drug-drug
interactions, 38t
Incision block, 48t
Increased transmission
mechanism, 8, 9t
Inflammatory arthritis
pain of, mechanisms of,
07
pathophysiology of,
0708
Inflammatory pain, 8t
cannabinoids for, 36
topical analgesics for, 7
Inhibition, descending,
modulators of, 9t
Intercostal nerve block, 49
Intra-articular block, 2, 48t
Intrathecal analgesia, 2
Irritable bowel, 8t
pain from, treatment
of, 22
Joint replacement, 2
Lacosamide, 2728, 86
adverse effects and side
effects of, 26t
for cancer pain, 96t
for cancer-related
neuropathic pain,
0
dosage and administration
of, 26t
mechanism of action
of, 26t
K
Keratinocytes, as drug
target, 7677
Ketamine, 6
adverse effects and side
effects of, 63
anti-hyperalgesic effect of,
663
contraindications to, 50
differential block of
sensory and
motor fibers,
552
dosage and administration
of, 5
duration of action,
505
and toxicological
profile, 50, 53
epidural analgesia with,
for postoperative
pain, 24, 25t
eutectic mixture of,
4950
guarded receptor
hypothesis for,
53, 54f
hydrophobicity of, 505,
53, 54f
inadvertent systemic
application of, 53
infusions, for
postoperative
pain, 24
intra-articular infusion,
for postoperative
pain, 25
liposomal formulations,
25
maximum daily dose
of, 55t
mechanism of action of,
0t, 4749
octanol-buffer coefficient
of, 53, 54f
onset of action, 505
and toxicological
profile, 50, 53
pharmacology of, 5052,
52t
for postoperative pain,
dosage and
administration of,
27t
precautions with, 50
safety of, 47
toxicity of, 5356
clinical signs of, 55, 56t
lipid rescue therapy for,
53, 5556
management protocols
for, 56
wound infiltration with,
24
Low back pain,
treatment of, 67, 27,
07, 0
Lumbar radicular pain,
treatment of, 27
Lumbar root pain, chronic,
45
Index
intravenous, 49, 53
for cancer pain, 96t
for cancer-related
neuropathic pain,
0
maximum daily dose
of, 55t
mechanism of action of,
74, 82t
molecular target of, 9t
onset of action, 52t
patch, 49, 74
pharmacology of, 50,
52t, 54f
plaster, 74
for neuropathic pain,
84
subcutaneous, for
cancer-related
neuropathic pain,
0
topical, 7475
adverse effects and side
effects of, 82t, 84
dosage and
administration of,
82t, 84
indications for, 7475
and lidocaine gel,
mixture of, 4950
for neuropathic pain,
82t, 84
and oral therapy,
combination
of, 75
pharmacology of, 74
for postherpetic
neuralgia, 74,
82t, 86
Lithium, and serotonergic
activity, 39t
Local anesthetics, 6, 47. See
also specific drug
administration of
routes for, 47, 48t
systemic, 47, 49
techniques for, 47, 48t
topical, 47, 48t, 4950
ultrasound-guided, 47
adverse effects and side
effects of
class A, 53
class B, 5355
amino amide, 50
pharmacology of, 52t
amino ester, 50
pharmacology of, 52t
anesthetic potency of,
505
anti-inflammatory action
of, 49
for cancer pain, 96t
in cancer treatment, 49
155
Laminectomy, 2
Lamotrigine, 9t, 27
and acetaminophen,
drug-drug
interactions, 36t
adverse effects and side
effects of, 25t
for cancer pain, 96t
for cancer-related
neuropathic pain,
0
carbamazepine and,
drug-drug
interactions, 33t
contraindications to, 25t
dosage and administration
of, 25t
for HIV-related
neuropathy, 88
mechanism of action
of, 25t
molecular target of, 9t
for neuropathic pain, 88
and phenytoin, drug-drug
interactions, 34t
precautions with, 25t
Leeds Assessment of
Neuropathic
Symptoms and
Signs (LANSS), 79
Leukopenia, drugs causing,
23
Levetiracetam, 9t, 27
adverse effects and side
effects of, 26t
dosage and administration
of, 26t
mechanism of action
of, 26t
Levobupivacaine
analgesic potency of, 52t
duration of action, 52t
maximum daily dose
of, 55t
onset of action, 52t
pharmacology of, 52t
for postoperative
pain, dosage
and administration
of, 27t
Levorphanol
adverse effects and side
effects of, 83t
dosage and administration
of, 83t
mechanism of action
of, 83t
for neuropathic pain,
83t, 88
precautions with, 83t
Lidocaine
analgesic potency of, 52t
duration of action, 52t, 53
Index
156
M
Macrolides, drug interactions
with, 8
Magnesium
as NMDA receptor
blocker, 6364
and perioperative pain
management,
6364
Maprotiline,
for neuropathic pain, 4
Marihuana (marijuana,
cannabis), 34t. See
also Cannabinoids
medical use of, 33,
vs. recreational use,
smoked
for HIV-related
neuropathy,
37, 88
for neuropathic pain,
3637
synthetic derivatives of,
33, 34t
Marinol. See Dronabinol
Massage,
MDMA
and serotonergic activity,
39t
and serotonin syndrome,
4
Memantine
for cancer pain, 96t
for cancer-related
neuropathic pain,
02
mechanism of action
of, 63
Menthol, 76
for rheumatic pain, 2
Meperidine
and other serotonergic
agents, drug-drug
interactions, 43
and serotonergic activity,
39t
Mepivacaine, 5253
analgesic potency of, 52t
duration of action, 52t
molecular structure of,
505, 5f
onset of action, 52t
pharmacology of, 50, 52t
Methadone
adverse effects and side
effects of, 83t
carbamazepine and,
drug-drug
interactions, 35t
clomipramine and,
drug-drug
interactions, 38t
dosage and administration
of, 83t
drug interactions with, 8
imipramine and,
drug-drug
interactions, 38t
indications for, 6, 6t
mechanism of action of,
63, 83t
mirtazapine and,
drug-drug
interactions, 38t
for neuropathic pain,
83t, 85
and other serotonergic
agents, drug-drug
interactions, 38t,
43
precautions with, 83t
St. John's wort and,
interactions
between, 42t
and serotonergic activity,
39t
and serotonin syndrome,
40
SSRIs and, drug-drug
interactions, 38t
trazodone and, drug-drug
interactions, 38t
venlafaxine and, drug-drug
interactions, 38t,
4
N-Methyl-D -aspartate
(NMDA)
receptor(s)
activation of, 60
in opioid-induced
hyperalgesia, 22
and -opioid receptors,
link between,
6, 6f
and postoperative
hyperalgesia,
606, 6f
N-Methyl-D -aspartate
(NMDA)
receptor blockers
(antagonists), 7t,
9t, 4, 3
for cancer pain, 96t
for cancer-related
neuropathic pain,
002
N
Nabilone, 3637
adverse effects and side
effects of,
for cancer pain, 96t, 00
dosage and administration
of, 34t
for fibromyalgia, 38, 09t,
pregabalin for, 0
sodium channel
blockers for, 0
sodium divalproex for,
0
subcutaneous lidocaine
for, 0
topiramate for, 0
treatment of, 22,
0002
tricyclic antidepressants
for, 8t
in cancer survivors,
000
cannabinoids for, 5, 34t,
3637, 8990
oromucosal, 8990
capsaicin patch for, 7,
83t, 8586
catastrophizing and, 90
central, 8688
duloxetine for, 88
characteristics of, 79
citalopram for, 4
clomipramine for,
placebocontrolled trials
of, 3t
combination therapy for,
7576, 8889
desipramine for, 4, 8t
placebo-controlled
trials of, 3t
diagnosis of, 7980
duloxetine for, 4, 7,
8084, 8t, 86
escitalopram for, 4
etiology of, 79
evoked, 79, 90
gabapentin for, 5, 7,
2223, 82t, 84,
86, 8889
in hemodialysis
patients, 23
and morphine,
combination
therapy with, 89
and nortriptyline,
combination
therapy with,
8889
and oxycodone,
combination
therapy with, 89
gabapentinoids for, 5, 7
imipramine for, 4, 88
placebo-controlled
trials of, 3t
intensity, temporal
variations in, 79
intermittent, 79
lamotrigine for, 88
levorphanol for, 83t, 88
Index
Neuralgia, 8t
Neuraxial block(s), 48, 48t,
24, 25t
Neurolytic block, 3
Neuropathic pain, 5, 8,
8t,
adjuvant analgesics for,
7, 7t
amitriptyline for, 4, 7,
80, 8t, 88
placebo-controlled
trials of, 3t
anticonvulsants for, 86
antidepressants for, 45
botulinum toxin type
Afor, 89
bupropion for, 4
calcium channel 2
ligands for, 82t, 84
cancer-related, 4. See
also Cancer pain
amantadine for, 02
amitriptyline for, 88
analgesics used for,
96t97t
anticonvulsants for, 0
antidepressants for, 0
baclofen for, 02
clonazepam for, 02
corticosteroids for,
9899
dextromethorphan
for, 02
gabapentin for, 82t, 0
gabapentin and
EMLA cream
for, combination
therapy with, 0
gabapentin and
imipramine for,
combination
therapy with, 0
gabapentin and opioids
for, combination
therapy with, 0
gabapentinoids for, 0
intravenous lidocaine
for, 0
ketamine for, 002
benzodiazepine with,
02
dosage and
administration of,
002
neuroleptic with, 02
lacosamide for, 0
lamotrigine for, 0
memantine for, 02
NMDA receptor
blockers
(antagonists) for,
002
oxcarbazepine for, 0
157
Index
158
O
Octreotide, 7t
for cancer pain, 97t
dosage and
administration
of, 99t
for cancer-related bowel
obstruction,
0304
Ofirmev, 2
Opioid(s), 9t. See also
Hyperalgesia,
opioid-induced;
specific drug
abuse, 4
adverse effects and side
effects of, 22
and cannabinoids
combination therapy
with, 40
interactions of, 40
for chronic noncancer
pain, 7
combinations of, efficacy
of, 3
dependence, 85
diversion, 4
dosage and administration
of, 3
indications for, 34, 8t
intraoperative, 606
long-term administration,
problems caused
by, 85
for neuropathic pain, 5
and NMDA receptor
activation, 60
P
Pain
acute
management of, 23,
36
topical diclofenac for, 72
arthritis. See Arthritis pain
bone. See Bone pain
cancer. See Cancer pain
central poststroke, 4,
27, 79
tricyclic antidepressants
for, 8t
chronic,
acute crises,
management of, 3
cannabinoids for, 34t,
3639
management of, 3, 34t,
3640, 6465
NMDA receptor
modulators for,
6465
postoperative, 26
without control,
management of, 3
definition of,
mild, treatment of, 2, 2f,
3, 6, 6t
moderate, treatment of,
2, 2f, 34, 6, 6t
musculoskeletal. See
Musculoskeletal
pain
neuropathic. See
Neuropathic pain
nonmalignant,
management of,
23
postamputation,
treatment of, 00
postmastectomy
gabapentin and
EMLA cream
combination
therapy for, 0
treatment of, 88, 98,
00
postsurgical, 79. See also
Postoperative pain
chronic, 26
treatment of, 23
postthoracotomy,
treatment of, 22,
00
rheumatic. See
Osteoarthritis;
Rheumatic pain;
Rheumatoid
arthritis (RA)
severe, treatment of, 2,
2f, 34, 6, 6t
PainDetect, 79
Pain emergencies, 99
Pain management
approaches to
interventional, 2
invasive, 23
nonpharmacological,
pharmacological, 23
physical,
psychological,
specific, 2
step down, 3
step up, 3
for chronic pain, 3. See
also Pain, chronic
step-down approach, 3
step-up approach, 3
goals of,
Pamidronate
for cancer pain, 97t
dosage and
administration
of, 99t
for cancer-related bone
pain, 0203
Index
Osteoclast inhibitor(s).
See also
Bisphosphonates
for cancer pain, 97t
dosage and
administration
of, 99t
for cancer-related bone
pain, 0203
Oxcarbazepine, 23, 86
adverse effects and side
effects of, 23, 25t
for cancer pain, 96t
for cancer-related
neuropathic pain,
0
contraindications to, 25t
dosage and administration
of, 25t
mechanism of action of,
0t, 25t
precautions with, 25t
Oxycodone
adverse effects and side
effects of, 83t
for chronic noncancer
pain, 7
dosage and administration
of, 83t, 85
high-dose, indications for,
6, 6t
low-dose, indications for,
6, 6t
mechanism of action of, 83t
for neuropathic pain, 5,
83t, 85
precautions with, 83t
159
Index
160
imipramine and,
drug-drug
interactions, 32t
lamotrigine and,
drug-drug
interactions, 34t
tricyclic antidepressants
and, drug-drug
interactions, 32t
Pirindole, for fibromyalgia,
5, 7
Plexus block, 48t, 49, 24,
25t
Polyneuropathy, 4, 27
Postherpetic neuralgia,
45, 7, 7986
capsaicin patch for, 83t
combination therapy
for, 89
gabapentin for, 22, 82t
nerve block for, 49
opioid agonists for, 83t,
85
pregabalin for, 22, 82t
topical capsaicin for,
7576, 8586
topical lidocaine for, 74,
82t, 84
treatment of, 2223, 86,
8889
tricyclic antidepressants
for, 8t
Postoperative pain
acetaminophen for, 2
dosage and
administration of,
27t
acute, 9
management of,
2026
ASA guidelines for,
9
multidisciplinary
approach to
(acute pain
service), 20
antidepressants for, 24
dosage and
administration of,
27t
balanced analgesia for,
2
bupivacaine for, dosage
and administration
of, 27t
celecoxib for, dosage and
administration of,
27t
chronic, 9, 26
prevalence of, 26
risk factors for, 26
COX2 inhibitors for,
222
Index
in hemodialysis
patients, 23
for osteoarthritis pain, 0
for painful diabetic
neuropathy, 22,
82t
perioperative use of, 23
pharmacology of, 222
for postherpetic neuralgia,
22, 82t
for postoperative pain,
2324
dosage and
administration of,
27t
for posttraumatic
neuropathy, 88
precautions with, 24t, 82t
for spinal cord
injury-related pain,
22, 8688
Prilocaine, 52
analgesic potency of, 52t
duration of action, 52t
and lignocaine, mixture of,
4950
maximum daily dose
of, 55t
onset of action, 52t
pharmacology of, 50, 52t
Procaine
analgesic potency of, 52t
duration of action, 52t
onset of action, 52t
pharmacology of, 50, 52t
PROSPECT working group,
26
Prostate cancer, skeletal
complications of,
denosumab for,
03
161
Index
162
Samarium-53, for
cancer-related
bone pain, 97t, 03
Sativex. See also Nabiximols
for rheumatic pain, 09t
for rheumatoid arthritis,
T
Tamoxifen, drug interactions
with, 8
Tapentadol
clomipramine and,
drug-drug
interactions, 38t
Index
163
Index
164
U
Ulnar nerve block, 48
Ultrasound,
V
Valproate, 28, 86
carbamazepine and,
drug-drug
interactions, 32t
Vanilloid receptor, subtype
, as drug target,
9t, 75, 85
Venlafaxine,
adverse effects and side
effects of, 2t,
8t, 4
and amitriptyline,
drug-drug
interactions, 4
for cancer pain, 96t, 98
dosage and administration
of, 2t, 8t, 84
half-life of, 2t
for headache, 57
mechanism of action
of, 8t
and methadone,
drug-drug
interactions, 38t,
4
for neuropathic pain,
4, 7, 8084,
8t, 88
placebo-controlled
trials of, 3t
neurotransmitter profile
of, 2t
and NSAIDs, drug-drug
interactions, 37t,
43
and other serotonergic
agents, drug-drug
interactions, 43
pharmacology of, 4
for postmastectomy
pain, 88
for postoperative pain,
dosage and
administration of,
27t
precautions with, 8t
St. John's wort and,
interactions
between, 42t
and serotonergic activity,
39t
W
Weight gain, drugs causing,
2t, 8
Withdrawal reaction(s), 6
World Health Organization
(WHO), analgesic
ladder/pain
ladder, 2, 2f,
56, 6t
modifications of, 23
Y
Yoga,
Z
Zolendronate
for cancer pain, 97t
for cancer-related bone
pain, 0203
Zonisamide, 2728
adverse effects and side
effects of, 26t
contraindications to, 26t
dosage and administration
of, 26t
mechanism of action
of, 26t
precautions with, 26